Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents

Transcription

Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
THE
FOURTH
REPORT
ON
THE
Diagnosis, Evaluation, and
Treatment of High Blood Pressure
in Children and Adolescents
U.S. DEPARTMENT OF HEALTH AND HUMAN SERVICES
National Institutes of Health
National Heart, Lung, and Blood Institute
T H E
F O U R T H
R E P O R T
O N
T H E
Diagnosis, Evaluation, and
Treatment of High Blood Pressure
in Children and Adolescents
U.S. DEPARTMENT OF HEALTH AND HUMAN SERVICES
National Institutes of Health
National Heart, Lung, and Blood Institute
NIH Publication No. 05-5267
Originally printed September 1996 (96-3790)
Revised May 2005
Acknowledgments
THE FOURTH REPORT ON
T H E D I A G N O S I S , E VA L U AT I O N ,
A N D T R E AT M E N T O F H I G H
BLOOD PRESSURE IN
CHILDREN AND ADOLESCENTS
CHAIR
Bonita Falkner, M.D. (Thomas Jefferson
University, Philadelphia, PA)
MEMBERS
Stephen R. Daniels, M.D., Ph.D.
(Cincinnati Children’s Hospital Medical
Center, Cincinnati, OH); Joseph T. Flynn,
M.D., M.S. (Montefiore Medical Center,
Bronx, NY); Samuel Gidding, M.D.
(DuPont Hospital for Children,
Wilmington, DE); Lee A. Green, M.D.,
M.P.H. (University of Michigan, Ann
Arbor, MI); Julie R. Ingelfinger, M.D.
(MassGeneral Hospital for Children,
Boston, MA); Ronald M. Lauer, M.D.
(University of Iowa, Iowa City, IA);
Bruce Z. Morgenstern, M.D. (Mayo
Clinic, Rochester, MN); Ronald J.
Portman, M.D. (The University of Texas
Health Science Center at Houston,
Houston, TX); Ronald J. Prineas, M.D.,
Ph.D. (Wake Forest University School
of Medicine, Winston-Salem, NC); Albert
P. Rocchini, M.D. (University of Michigan,
C.S. Mott Children’s Hospital, Ann Arbor,
MI); Bernard Rosner, Ph.D. (Harvard
School of Public Health, Boston, MA);
Alan Robert Sinaiko, M.D. (University of
Minnesota Medical School, Minneapolis,
MN); Nicolas Stettler, M.D., M.S.C.E.
(The Children’s Hospital of Philadelphia,
Philadelphia, PA); Elaine Urbina, M.D.
(Cincinnati Children’s Hospital Medical
Center, Cincinnati, OH)
N AT I O N A L I N S T I T U T E S O F
H E A LT H S T A F F
Edward J. Roccella, Ph.D., M.P.H.
(National Heart, Lung, and Blood
Institute, Bethesda, MD); Tracey Hoke,
M.D., M.Sc. (National Heart, Lung, and
Blood Institute, Bethesda, MD); Carl E.
Hunt, M.D. (National Center on Sleep
Disorders Research, National Heart,
Lung, and Blood Institute, Bethesda,
MD); Gail Pearson, M.D., Sc.D.
(National Heart, Lung, and Blood
Institute, Bethesda, MD)
STAFF
Joanne Karimbakas, M.S., R.D., and
Ann Horton, M.S. (American Institutes
for Research Health Program, Silver
Spring, MD)
FINANCIAL DISCLOSURES
Dr. Flynn has served as a consultant/
advisor for Pfizer Inc., AstraZeneca LP,
ESP-Pharma, and Novartis Pharmaceuticals;
he received funding/grant support for
research projects from Pfizer, AstraZeneca,
and Novartis.
ACKNOWLEDGMENTS
We would like to thank the American
Academy of Pediatrics for its help in disseminating this report. We appreciate the
assistance by: Carol Creech, M.I.L.S.,
Heather Banks, M.A., and Angela Jehle
(American Institutes for Research Health
Program, Silver Spring, MD).
Acknowledgments
iii
T H E N AT I O N A L H I G H B L O O D
P R E S S U R E E D U C AT I O N
P R O G R A M C O O R D I N AT I N G
COMMITTEE MEMBER
O R G A N I Z AT I O N S
American Academy of Family Physicians
American Academy of Insurance Medicine
American Academy of Neurology
American Academy of Ophthalmology
American Academy of Physician Assistants
American Association of Occupational
Health Nurses
American College of Cardiology
American College of Chest Physicians
American College of Occupational
and Environmental Medicine
American College of Physicians–
American Society of Internal Medicine
American College of Preventive Medicine
American Dental Association
American Diabetes Association
American Dietetic Association
American Heart Association
American Hospital Association
American Medical Association
American Nurses Association
American Optometric Association
American Osteopathic Association
American Pharmaceutical Association
American Podiatric Medical Association
American Public Health Association
American Red Cross
iv
American Society of Health-System
Pharmacists
American Society of Hypertension
American Society of Nephrology
Association of Black Cardiologists
Citizens for Public Action on High Blood
Pressure and Cholesterol, Inc.
Hypertension Education Foundation, Inc.
International Society on Hypertension
in Blacks
National Black Nurses Association, Inc.
National Heart, Lung, and Blood Institute
Ad Hoc Committee on Minority
Populations
National Hypertension Association, Inc.
National Kidney Foundation, Inc.
National Medical Association
National Optometric Association
National Stroke Association
Society for Nutrition Education
The Society of Geriatric Cardiology
Federal Agencies:
Agency for Healthcare Research and Quality
Centers for Medicare and Medicaid Services
Department of Veterans Affairs
Health Resources and Services Administration
National Center for Health Statistics
National Heart, Lung, and Blood Institute
National Institute of Diabetes and Digestive
and Kidney Diseases
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Contents
FOREWORD
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .VII
INTRODUCTION
METHODS
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .1
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .3
DEFINITION OF HYPERTENSION
. . . . . . . . . . . . . . . . . . . . . . . . . . . .4
MEASUREMENT OF BLOOD PRESSURE IN CHILDREN
Ambulatory Blood Pressure Monitoring
B L O O D P R E S S U R E TA B L E S
Using the Blood Pressure Tables
. . . . . . . . . . .5
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .7
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .8
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .9
P R I M A R Y H Y P E R T E N S I O N A N D E VA L U AT I O N
FOR COMORBIDITIES . . . . . . . . . . . . . . . . . . . .
. . . . . . . . . . . . . . . . .16
E VA L U AT I O N F O R S E C O N D A R Y H Y P E R T E N S I O N
. . . . . . . . . . .1
8
Physical Examination . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .18
Additional Diagnostic Studies for Hypertension . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .19
Renin Profiling . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .19
Evaluation for Possible Renovascular Hypertension . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .19
Invasive Studies . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .19
T A R G E T- O R G A N A B N O R M A L I T I E S
IN CHILDHOOD HYPERTENSION .
Clinical Recommendation
. . . . . . . . . . . . . . . . . . . . . . . . . .22
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .23
THERAPEUTIC LIFESTYLE CHANGES
PHARMACOLOGIC THERAPY
OF CHILDHOOD HYPERTENSION
. . . . . . . . . . . . . . . . . . . . . . .24
. . . . . . . . . . . . . . . . . . . . . . . . . . .26
A P P E N D I X A . D E M O G R A P H I C D ATA
. . . . . . . . . . . . . . . . . . . . . . . .34
A P P E N D I X B . C O M P U TAT I O N O F B L O O D
PRESSURE PERCENTILES FOR ARBITRARY
SEX, AGE, AND HEIGHT . . . . . . . . . . . . . . . .
S C H E M E U S E D F O R C L A S S I F I C AT I O N
OF THE EVIDENCE . . . . . . . . . . . . . . . .
REFERENCES
. . . . . . . . . . . . . . . . . .36
. . . . . . . . . . . . . . . . . . . . . . .39
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .40
Contents
v
List of Tables
TA B L E 1 .
Conditions Under Which Children <3 Years Old Should Have . . . . . . . . . . . . . . .5
Blood Pressure Measured . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
TA B L E 2 .
Recommended Dimensions for Blood Pressure Cuff Bladders
TA B L E 3 .
Blood Pressure Levels for Boys by Age and Height Percentile
. . . . . . . . . . .10
TA B L E 4 .
Blood Pressure Levels for Girls by Age and Height Percentile
. . . . . . . . . . .12
TA B L E 5 .
Classification of Hypertension in Children and Adolescents, . . . . . . . . . . . .14
With Measurement Frequency and Therapy Recommendations . . . . . . .
TA B L E 6 .
Indications for Antihypertensive Drug Therapy in Children
TA B L E 7 .
Clinical Evaluation of Confirmed Hypertension . . . . . . . . . . . . . . . . . . . . . . . . . . .15
TA B L E 8 .
Examples of Physical Examination Findings Suggestive . . . . . . . . . . . . . . . . .20
of Definable Hypertension . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
TA B L E 9 .
Antihypertensive Drugs for Outpatient Management . . . . . . . . . . . . . . . . . . . . .28
of Hypertension in Children 1–17 Years Old . . . . . . . . . . . . . . . . . . . . .
TA B L E 1 0 .
Antihypertensive Drugs for Management of Severe Hypertension . . . . . . .33
in Children 1–17 Years Old . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
TA B L E A – 1 .
Demographic Data on Height/Blood Pressure Distribution Curves . . . . . .35
by Study Population . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
TA B L E B – 1 .
Regression Coefficients From Blood Pressure Regression Models
. . . . . . . . . . . . . . . .6
. . . . . . . . . . . . .14
. . . . . . .38
List of Figures
FIGURE 1.
vi
Management Algorithm . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .32
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Foreword
This is the fourth report from the National
High Blood Pressure Education Program
(NHBPEP) Working Group on Children
and Adolescents; it updates the previous publication, Update on the Task Force Report
(1987) on High Blood Pressure in Children
and Adolescents (Pediatrics. 1996;98:649–58).
The purpose of this report is to update clinicians on the latest recommendations
concerning the diagnosis, evaluation, and
treatment of hypertension in children; recommendations are based on English-language,
peer-reviewed, scientific evidence (from 1997
to 2004) and the consensus expert opinion of
the NHBPEP Working Group.
This report includes new data from the
1999–2000 National Health and Nutrition
Examination Survey (NHANES), as well as
revised blood pressure (BP) tables that include
the 50th, 90th, 95th, and 99th percentiles by
sex, age, and height. Hypertension in children
and adolescents continues to be defined as
systolic BP (SBP) and/or diastolic BP (DBP)
that is, on repeated measurement, at or above
the 95th percentile for sex, age, and height.
BP between the 90th and 95th percentile in
childhood is now termed “prehypertension”
and is an indication for lifestyle modifications.
New guidelines are provided for the staging of
hypertension in children and adolescents, as
well as updated recommendations for diagnostic evaluation of hypertensive children.
In addition, the report evaluates the evidence
of early target-organ damage in children and
adolescents with hypertension; provides the
rationale for early identification and treatment; and provides revised recommendations,
based on recent studies, for the use of antihypertensive drug therapy. Treatment recommendations also include updated evaluation
of nonpharmacologic therapies to reduce
additional cardiovascular risk factors. The
report describes how to identify hypertensive
children who need additional evaluation for
sleep disorders that may be associated with
BP elevation.
Dr. Bonita Falkner has our deep appreciation
for leading the members of the NHBPEP
Working Group in developing this new report.
Dr. Falkner and the Working Group performed diligently and brilliantly to assemble
this document in a timely manner. Applying
these recommendations to clinical practice will
address the important public health issue of
improving inadequate BP control.
Barbara M. Alving, M.D.
Acting Director
National Heart, Lung, and Blood Institute
and
Chair
National High Blood Pressure Education Program
Coordinating Committee
Foreword
vii
Introduction
Considerable advances have been made in
detection, evaluation, and management of
high blood pressure, or hypertension, in children and adolescents. Because of the
development of a large national database
on normative blood pressure (BP) levels
throughout childhood, the ability to identify
children who have abnormally elevated BP
has improved. On the basis of developing
evidence, it is now apparent that primary
hypertension is detectable in the young and
occurs commonly. The long-term health risks
for hypertensive children and adolescents can
be substantial; therefore, it is important that
clinical measures be taken to reduce these
risks and optimize health outcomes.
The purpose of this report is to update clinicians on the latest scientific evidence
regarding BP in children and to provide recommendations for diagnosis, evaluation, and
treatment of hypertension based on available
evidence and consensus expert opinion of the
Working Group when evidence was lacking.
This publication is the fourth report from the
National High Blood Pressure Education
Program (NHBPEP) Working Group on
Children and Adolescents and updates the
previous 1996 publication, Update on the
Task Force Report (1987) on High Blood
Pressure in Children and Adolescents.1
This report includes the following information:
■ New data, from the 1999–2000 National
Health and Nutrition Examination Survey
(NHANES), have been added to the child-
hood BP database, and the BP data have
been reexamined. The revised BP tables
now include the 50th, 90th, 95th, and
99th percentiles by sex, age, and height.
■
■
■
■
■
Hypertension in children and adolescents
continues to be defined as systolic BP (SBP)
and/or diastolic BP (DBP) that is, on
repeated measurement, at or above the 95th
percentile. BP between the 90th and 95th
percentile in childhood had been designated
“high normal.” To be consistent with the
Seventh Report of the Joint National
Committee on the Prevention, Detection,
Evaluation, and Treatment of High Blood
Pressure (JNC 7), this level of BP will now
be termed “prehypertensive” and is an indication for lifestyle modifications.2
The evidence of early target-organ damage
in children and adolescents with hypertension is evaluated, and the rationale for early
identification and treatment is provided.
Based on recent studies, revised recommendations for use of antihypertensive drug
therapy are provided.
Treatment recommendations include
updated evaluation of nonpharmacologic
therapies to reduce additional cardiovascular risk factors.
Information is included on the identification
of hypertensive children who need additional evaluation for sleep disorders.
Introduction
1
Methods
In response to the request of the NHBPEP
Chair and Director of the National Heart,
Lung, and Blood Institute (NHLBI) regarding
the need to update the JNC 7 report,2 some
NHBPEP Coordinating Committee members
suggested that the NHBPEP Working Group
Report on Hypertension in Children and
Adolescents should be revisited. Thereafter,
the NHLBI Director directed the NHLBI staff
to examine issues that might warrant a new
report on children. Several prominent clinicians and scholars were asked to develop
background manuscripts on selected issues
related to hypertension in children and adolescents. Their manuscripts synthesized the
available scientific evidence. During the
spring and summer of 2002, NHLBI staff and
the chair of the 1996 NHBPEP Working
Group report on hypertension in children and
adolescents reviewed the scientific issues
addressed in the background manuscripts as
well as contemporary policy issues. Subsequently, the staff noted that a critical mass
of new information had been identified, thus
warranting the appointment of a panel to
update the earlier NHBPEP Working Group
Report. The NHLBI Director appointed the
authors of the background papers and other
national experts to serve on the new panel.
The chair and NHLBI staff developed a
report outline and timeline to complete the
work in 5 months.
The background papers served as focal points
for review of the scientific evidence at the first
meeting. The members of the Working Group
were assembled into teams, and each team
prepared specific sections of the report. In
developing the focus of each section, the
Working Group was asked to consider the
peer-reviewed scientific literature published in
English since 1997. The scientific evidence
was classified by the system used in the
JNC 7.2 The chair assembled the sections
submitted by each team into the first draft of
the report. The draft report was distributed
to the Working Group for review and comment. These comments were assembled and
used to create the second draft. A subsequent
onsite meeting of the Working Group was
conducted to discuss further revisions and the
development of the third draft document.
Amended sections were reviewed, critiqued,
and incorporated into the third draft. After
editing by the chair for internal consistency,
the fourth draft was created. The Working
Group reviewed this draft, and conference
calls were conducted to resolve any remaining
issues that were identified. When the Working
Group approved the final document, it was
distributed to the Coordinating Committee
for review.
Methods
3
Definition of Hypertension
■
■
■
■
Hypertension is defined as average SBP and/or DBP that is greater than or equal
to the 95th percentile for sex, age, and height on three or more occasions.
Prehypertension in children is defined as average SBP or DBP levels that are greater
than or equal to the 90th percentile, but less than the 95th percentile.
As with adults, adolescents with BP levels greater than or equal to 120/80 mmHg
should be considered prehypertensive.
A patient with BP levels above the 95th percentile in a physician’s office or clinic,
who is normotensive outside a clinical setting, has white-coat hypertension.
Ambulatory BP monitoring (ABPM) is usually required to make this diagnosis.
The definition of hypertension in children and
adolescents is based on the normative distribution of BP in healthy children. Normal BP
is defined as SBP and DBP that is less than the
90th percentile for sex, age, and height.
Hypertension is defined as average SBP or
DBP that is greater than or equal to the
95th percentile for sex, age, and height on at
least three separate occasions. Average SBP or
DBP levels that are greater than or equal to
the 90th percentile, but less than the 95th percentile, had been designated as “high normal”
and were considered to be an indication of
heightened risk for developing hypertension.
This designation is consistent with the
description of “prehypertension” in adults.
The JNC 7 Committee now defines prehyper-
4
tension as a BP level that is equal to or greater
than 120/80 mmHg and recommends the
application of preventive health-related
behaviors, or therapeutic lifestyle changes,
for individuals having SBP levels that exceed
120 mmHg.2 It is now recommended that,
as with adults, children and adolescents with
BP levels at 120/80 mmHg or above, but less
than the 95th percentile, should be considered
prehypertensive.
The term white-coat hypertension defines a
clinical condition in which the patient has BP
levels that are above the 95th percentile when
measured in a physician’s office or clinic,
whereas the patient’s average BP is below the
90th percentile outside of a clinical setting.
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Measurement of
Blood Pressure in Children
■
■
■
■
■
Children >3 years old who are seen in a medical setting should have their BP
measured.
The preferred method of BP measurement is auscultation.
Correct measurement requires a cuff that is appropriate to the size of the child’s
upper arm.
Elevated BP must be confirmed on repeated visits before characterizing a child
as having hypertension.
Measures obtained by oscillometric devices that exceed the 90th percentile should
be repeated by auscultation.
Children over the age of 3 years who are seen
in medical care settings should have their BP
measured at least once during every health
care episode. Children under age 3 should
have their BP measured in special circumstances. (See table 1.)
The BP tables are based on auscultatory
measurements; therefore, the preferred
method of measurement is auscultation.
As discussed below, oscillometric devices are
convenient and minimize observer error, but
they do not provide measures that are identical to auscultation. To confirm hypertension,
the BP in children should be measured with a
standard clinical sphygmomanometer, using a
stethoscope placed over the brachial artery
pulse, proximal and medial to the cubital
fossa, and below the bottom edge of the cuff
(i.e., about 2 cm above the cubital fossa). The
use of the bell of the stethoscope may allow
softer Korotkoff sounds to be heard better.3,4
The use of an appropriately sized cuff may
preclude the placement of the stethoscope
in this precise location, but there is little
evidence that significant inaccuracy is introduced, either if the head of the stethoscope
is slightly out of position or if there is contact
between the cuff and the stethoscope. Preparation of the child for standard measurement
can affect the BP level just as much as
technique.5 Ideally, the child whose BP is to
be measured should have avoided stimulant
drugs or foods, have been sitting quietly for
5 minutes, and seated with his or her back
supported, feet on the floor and right arm
supported, cubital fossa at heart level.6,7 The
right arm is preferred in repeated measures of
BP for consistency and comparison to standard tables and because of the possibility of
TABLE
1
Conditions Under Which Children
<3 Years Old Should Have Blood
Pressure Measured
■
■
■
■
■
■
■
■
■
■
History of prematurity, very low
birthweight, or other neonatal complication
requiring intensive care
Congenital heart disease (repaired or
nonrepaired)
Recurrent urinary tract infections,
hematuria, or proteinuria
Known renal disease or urologic
malformations
Family history of congenital renal disease
Solid organ transplant
Malignancy or bone marrow transplant
Treatment with drugs known to raise BP
Other systemic illnesses associated with
hypertension (neurofibromatosis, tuberous
sclerosis, etc.)
Evidence of elevated intracranial pressure
Measurement of Blood Pressure in Children
5
TABLE
2
Recommended Dimensions for Blood Pressure Cuff Bladders
Age Range
Width (cm) Length (cm)
Maximum Arm
Circumference (cm)*
Newborn
4
8
10
Infant
6
12
15
Child
9
18
22
Small adult
10
24
26
Adult
13
30
34
Large adult
16
38
44
Thigh
20
42
52
* Calculated so that the largest arm would still allow bladder to encircle arm by at least 80 percent.
coarctation of the aorta, which might lead to
false (low) readings in the left arm.8
Correct measurement of BP in children
requires use of a cuff that is appropriate to
the size of the child’s upper right arm. The
equipment necessary to measure BP in children, ages 3 through adolescence, includes
child cuffs of different sizes and must also
include a standard adult cuff, a large adult
cuff, and a thigh cuff. The latter two cuffs
may be needed for use in adolescents.
By convention, an appropriate cuff size is a
cuff with an inflatable bladder width that is at
least 40 percent of the arm circumference at a
point midway between the olecranon and the
acromion. (See www.americanheart.org/presenter.jhtml?identifier=576.)9,10 For such a
cuff to be optimal for an arm, the cuff
bladder length should cover 80–100 percent
of the circumference of the arm.1,11 Such a
requirement demands that the bladder widthto-length ratio be at least 1:2. Not all
commercially available cuffs are manufactured with this ratio. Additionally, cuffs
labeled for certain age populations (e.g.,
infant cuffs, child cuffs) are constructed with
widely disparate dimensions. Accordingly, the
Working Group recommends that standard
cuff dimensions for children be adopted. (See
table 2.) BP measurements are overestimated
to a greater degree with a cuff that is too
small than they are underestimated by a cuff
that is too large. If a cuff is too small, the
6
next largest cuff should be used, even if it
appears large. If the appropriate cuffs are
used, the cuff size effect is obviated.12
SBP is determined by the onset of the “tapping” Korotkoff sounds (K1). Population
data in children1 and risk-associated epidemiological data in adults13 have established the
fifth Korotkoff sound (K5), or the disappearance of Korotkoff sounds, as the definition of
DBP. In some children, Korotkoff sounds can
be heard to 0 mmHg. Under these circumstances, the BP measurement should be
repeated with less pressure on the head of the
stethoscope.4 Only if the very low K5 persists
should K4 (muffling of the sounds) be
recorded as the DBP.
The standard device for BP measurements has
been the mercury manometer.14 Because of its
environmental toxicity, mercury has been
increasingly removed from health care settings. Aneroid manometers are quite accurate
when calibrated on a semiannual basis15 and
are recommended when mercury-column
devices cannot be obtained.
Auscultation remains the recommended
method of BP measurement in children, under
most circumstances. Oscillometric devices
measure mean arterial BP and then calculate
systolic and diastolic values.16 The algorithms
used by companies are proprietary and differ
from company to company and device to
device. These devices can yield results that
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
vary widely when one is compared with
another,17 and they do not always closely
match BP values obtained by auscultation.18
Oscillometric devices must be validated on a
regular basis. Protocols for validation have
been developed,19,20 but the validation process
is very difficult.
Two advantages of automatic devices are their
ease of use and the minimization of observer
bias or digit preference.16 Use of the automated devices is preferred for BP measurement
in newborns and young infants, in whom
auscultation is difficult, and in the intensive
care setting where frequent BP measurement
is needed. An elevated BP reading obtained
with an oscillometric device should be
repeated using auscultation.
Elevated BP must be confirmed on repeated
visits before characterizing a child as having
hypertension. Confirming an elevated BP
measurement is important, because BP at high
levels tends to fall on subsequent measurement as the result of (1) an accommodation
effect (i.e., reduction of anxiety by the patient
from one visit to the next), and (2) regression
to the mean. BP level is not static but varies
even under standard resting conditions.
Therefore, except in the presence of severe
hypertension, a more precise characterization
of a person’s BP level is an average of multiple
BP measurements taken over weeks to months.
A M B U L AT O R Y B L O O D
PRESSURE MONITORING
Ambulatory BP monitoring (ABPM) refers to
a procedure in which a portable BP device,
worn by the patient, records BP over a specified period, usually 24 hours. ABPM is very
useful in the evaluation of hypertension in
children.21–23 By frequent measurement and
recording of BP, ABPM enables computation
of the mean BP during the day, night, and
over 24 hours as well as various measures to
determine the degree to which BP exceeds the
upper limit of normal over a given time
period (i.e., the BP load). ABPM is especially
helpful in the evaluation of white-coat hypertension, as well as the risk for hypertensive
organ injury, apparent drug resistance, and
hypotensive symptoms with antihypertensive
drugs. ABPM is also useful for evaluating
patients for whom more information on BP
patterns is needed, such as those with episodic
hypertension, chronic kidney disease, diabetes,
and autonomic dysfunction. Conducting
ABPM requires specific equipment and trained
staff. Therefore, ABPM in children and adolescents should be used by experts in the field
of pediatric hypertension who are experienced
in its use and interpretation.
Measurement of Blood Pressure in Children
7
Blood Pressure Tables
■
■
BP standards based on sex, age, and height provide a precise classification
of BP according to body size.
The revised BP tables now include the 50th, 90th, 95th, and 99th percentiles
(with standard deviations) by sex, age, and height.
In children and adolescents, the normal range
of BP is determined by body size and age.
BP standards that are based on sex, age, and
height provide a more precise classification
of BP according to body size. This approach
avoids misclassifying children who are very
tall or very short.
The BP tables are revised to include the
new height percentile data (www.cdc.gov/
growthcharts/)24 as well as the addition of BP
data from the NHANES 1999–2000. Demographic information on the source of the BP
data is provided in appendix A. The 50th,
90th, 95th, and 99th percentiles of SBP and
DBP (using K5) for height by sex and age are
given for boys and girls in tables 3 and 4.
Although new data have been added, the sex,
age, and height BP levels for the 90th and
95th percentiles have changed minimally from
the last report. The 50th percentile has been
added to the tables to provide the clinician
with the BP level at the midpoint of the
normal range. Although the 95th percentile
provides a BP level that defines hypertension,
management decisions about children with
hypertension should be determined by the
degree or severity of hypertension. Therefore,
the 99th percentile has been added to facilitate clinical decisionmaking in the plan for
evaluation. Standards for SBP and DBP for
infants younger than 1 year are available.25
In children younger than 1 year, SBP has been
used to define hypertension.
To use the tables in a clinical setting, the
height percentile is determined by using the
8
newly revised CDC Growth Charts
(www.cdc.gov/growthcharts/). The child’s
measured SBP and DBP are compared with
the numbers provided in the table (boys or
girls) according to the child’s age and height
percentile. The child is normotensive if the
BP is below the 90th percentile. If the BP is
equal to or above the 90th percentile, the BP
measurement should be repeated at that visit
to verify an elevated BP. BP measurements
between the 90th and 95th percentiles indicate prehypertension and warrant reassessment
and consideration of other risk factors. (See
table 5.) In addition, if an adolescent’s BP is
greater than 120/80 mmHg, the patient
should be considered to be prehypertensive
even if this value is less than the 90th percentile. This BP level typically occurs for SBP
at age 12 years and for DBP at age 16 years.
If the child’s BP (systolic or diastolic) is at or
above the 95th percentile, the child may be
hypertensive, and the measurement must be
repeated on at least two additional occasions
to confirm the diagnosis. Staging of BP,
according to the extent to which a child’s BP
exceeds the 95th percentile, is helpful in developing a management plan for evaluation and
treatment that is most appropriate for an individual patient. On repeated measurement,
hypertensive children may have BP levels that
are only a few mmHg above the 95th percentile; these children would be managed
differently from hypertensive children who
have BP levels that are 15–20 mmHg above
the 95th percentile. An important clinical
decision is to determine which hypertensive
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
children require more immediate attention for
elevated BP. The difference between the 95th
and 99th percentiles is only 7–10 mmHg and
is not large enough, particularly in view of the
variability in BP measurements, to adequately
distinguish mild hypertension—where limited
evaluation is most appropriate—from more
severe hypertension where more immediate
and extensive intervention is indicated.
Therefore, Stage 1 hypertension is the designation for BP levels that range from the 95th
percentile to 5 mmHg above the 99th percentile. Stage 2 hypertension is the designation
for BP levels that are higher than 5 mmHg
above the 99th percentile. Once confirmed
on repeated measures, Stage 1 hypertension
allows time for evaluation before initiating
treatment unless the patient is symptomatic.
Patients with Stage 2 hypertension may need
more prompt evaluation and pharmacologic
therapy. Symptomatic patients with Stage 2
hypertension require immediate treatment and
consultation with experts in pediatric hypertension. These categories are parallel to the
staging of hypertension in adults, as noted in
JNC 7.2
USING THE BLOOD
PRESSURE TABLES
1. Use the standard height charts to determine
the height percentile.
2. Measure and record the child’s SBP
and DBP.
5. There, find the 50th, 90th, 95th, and 99th
percentiles for SBP in the left columns and
for DBP in the right columns.
■
■
■
BP less than the 90th percentile is normal.
BP between the 90th and 95th percentile
is prehypertension. In adolescents, BP
equal to or exceeding 120/80 mmHg is
prehypertension, even if this figure is less
than the 90th percentile.
BP greater than the 95th percentile may
be hypertension.
6. If the BP is greater than the 90th percentile,
the BP should be repeated twice at the
same office visit, and an average SBP and
DBP should be used.
7. If the BP is greater than the 95th percentile,
BP should be staged. If Stage 1 (95th
percentile to the 99th percentile plus
5 mmHg), BP measurements should be
repeated on two more occasions. If hypertension is confirmed, evaluation should
proceed as described in table 7. If BP is
Stage 2 (>99th percentile plus 5 mmHg),
prompt referral should be made for
evaluation and therapy. If the patient is
symptomatic, immediate referral and treatment are indicated. Those patients with a
compelling indication, as noted in table 6,
would be treated as the next higher category of hypertension.
3. Use the correct gender table for SBP
and DBP.
4. Find the child’s age on the left side of the
table. Follow the age row horizontally
across the table to the intersection of the
line for the height percentile (vertical
column).
Blood Pressure Tables
9
TABLE
3
Blood Pressure Levels for Boys by Age and Height Percentile*
Age
(Year)
1
2
3
4
5
6
7
8
9
10
10
Systolic BP (mmHg)
Diastolic BP (mmHg)
← Percentile of Height →
← Percentile of Height →
BP
Percentile
↓
5th
10th
25th
50th
75th
90th
95th
5th
10th
25th
50th
75th
90th
95th
50th
80
81
83
85
87
88
89
34
35
36
37
38
39
39
90th
94
95
97
99
100
102
103
49
50
51
52
53
53
54
95th
98
99
101
103
104
106
106
54
54
55
56
57
58
58
99th
105
106
108
110
112
113
114
61
62
63
64
65
66
66
50th
84
85
87
88
90
92
92
39
40
41
42
43
44
44
90th
97
99
100
102
104
105
106
54
55
56
57
58
58
59
95th
101
102
104
106
108
109
110
59
59
60
61
62
63
63
99th
109
110
111
113
115
117
117
66
67
68
69
70
71
71
50th
86
87
89
91
93
94
95
44
44
45
46
47
48
48
90th
100
101
103
105
107
108
109
59
59
60
61
62
63
63
95th
104
105
107
109
110
112
113
63
63
64
65
66
67
67
99th
111
112
114
116
118
119
120
71
71
72
73
74
75
75
50th
88
89
91
93
95
96
97
47
48
49
50
51
51
52
90th
102
103
105
107
109
110
111
62
63
64
65
66
66
67
95th
106
107
109
111
112
114
115
66
67
68
69
70
71
71
99th
113
114
116
118
120
121
122
74
75
76
77
78
78
79
50th
90
91
93
95
96
98
98
50
51
52
53
54
55
55
90th
104
105
106
108
110
111
112
65
66
67
68
69
69
70
95th
108
109
110
112
114
115
116
69
70
71
72
73
74
74
99th
115
116
118
120
121
123
123
77
78
79
80
81
81
82
50th
91
92
94
96
98
99
100
53
53
54
55
56
57
57
90th
105
106
108
110
111
113
113
68
68
69
70
71
72
72
95th
109
110
112
114
115
117
117
72
72
73
74
75
76
76
99th
116
117
119
121
123
124
125
80
80
81
82
83
84
84
50th
92
94
95
97
99
100
101
55
55
56
57
58
59
59
90th
106
107
109
111
113
114
115
70
70
71
72
73
74
74
95th
110
111
113
115
117
118
119
74
74
75
76
77
78
78
99th
117
118
120
122
124
125
126
82
82
83
84
85
86
86
50th
94
95
97
99
100
102
102
56
57
58
59
60
60
61
90th
107
109
110
112
114
115
116
71
72
72
73
74
75
76
95th
111
112
114
116
118
119
120
75
76
77
78
79
79
80
99th
119
120
122
123
125
127
127
83
84
85
86
87
87
88
50th
95
96
98
100
102
103
104
57
58
59
60
61
61
62
90th
109
110
112
114
115
117
118
72
73
74
75
76
76
77
95th
113
114
116
118
119
121
121
76
77
78
79
80
81
81
99th
120
121
123
125
127
128
129
84
85
86
87
88
88
89
50th
97
98
100
102
103
105
106
58
59
60
61
61
62
63
90th
111
112
114
115
117
119
119
73
73
74
75
76
77
78
95th
115
116
117
119
121
122
123
77
78
79
80
81
81
82
99th
122
123
125
127
128
130
130
85
86
86
88
88
89
90
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Age
(Year)
11
12
13
14
15
16
17
Systolic BP (mmHg)
Diastolic BP (mmHg)
← Percentile of Height →
← Percentile of Height →
BP
Percentile
↓
5th
10th
25th
50th
75th
90th
95th
5th
10th
25th
50th
75th
90th
95th
50th
99
100
102
104
105
107
107
59
59
60
61
62
63
63
90th
113
114
115
117
119
120
121
74
74
75
76
77
78
78
95th
117
118
119
121
123
124
125
78
78
79
80
81
82
82
99th
124
125
127
129
130
132
132
86
86
87
88
89
90
90
50th
101
102
104
106
108
109
110
59
60
61
62
63
63
64
90th
115
116
118
120
121
123
123
74
75
75
76
77
78
79
95th
119
120
122
123
125
127
127
78
79
80
81
82
82
83
99th
126
127
129
131
133
134
135
86
87
88
89
90
90
91
50th
104
105
106
108
110
111
112
60
60
61
62
63
64
64
90th
117
118
120
122
124
125
126
75
75
76
77
78
79
79
95th
121
122
124
126
128
129
130
79
79
80
81
82
83
83
99th
128
130
131
133
135
136
137
87
87
88
89
90
91
91
50th
106
107
109
111
113
114
115
60
61
62
63
64
65
65
90th
120
121
123
125
126
128
128
75
76
77
78
79
79
80
95th
124
125
127
128
130
132
132
80
80
81
82
83
84
84
99th
131
132
134
136
138
139
140
87
88
89
90
91
92
92
50th
109
110
112
113
115
117
117
61
62
63
64
65
66
66
90th
122
124
125
127
129
130
131
76
77
78
79
80
80
81
95th
126
127
129
131
133
134
135
81
81
82
83
84
85
85
99th
134
135
136
138
140
142
142
88
89
90
91
92
93
93
50th
111
112
114
116
118
119
120
63
63
64
65
66
67
67
90th
125
126
128
130
131
133
134
78
78
79
80
81
82
82
95th
129
130
132
134
135
137
137
82
83
83
84
85
86
87
99th
136
137
139
141
143
144
145
90
90
91
92
93
94
94
50th
114
115
116
118
120
121
122
65
66
66
67
68
69
70
90th
127
128
130
132
134
135
136
80
80
81
82
83
84
84
95th
131
132
134
136
138
139
140
84
85
86
87
87
88
89
99th
139
140
141
143
145
146
147
92
93
93
94
95
96
97
BP, blood pressure
* The 90th percentile is 1.28 SD, 95th percentile is 1.645 SD, and the 99th percentile is 2.326 SD over the mean. For research purposes,
the standard deviations in appendix table B–1 allow one to compute BP Z-scores and percentiles for boys with height percentiles given
in table 3 (i.e., the 5th, 10th, 25th, 50th, 75th, 90th, and 95th percentiles). These height percentiles must be converted to height
Z-scores given by (5% = -1.645; 10% = -1.28; 25% = -0.68; 50% = 0; 75% = 0.68; 90% = 1.28; 95% = 1.645) and then computed
according to the methodology in steps 2–4 described in appendix B. For children with height percentiles other than these, follow steps
1–4 as described in appendix B.
Blood Pressure Tables
11
TABLE
4
Blood Pressure Levels for Girls by Age and Height Percentile*
Age
(Year)
1
2
3
4
5
6
7
8
9
10
12
Systolic BP (mmHg)
Diastolic BP (mmHg)
← Percentile of Height →
← Percentile of Height →
BP
Percentile
↓
5th
10th
25th
50th
75th
90th
95th
5th
10th
25th
50th
75th
90th
95th
50th
83
84
85
86
88
89
90
38
39
39
40
41
41
42
90th
97
97
98
100
101
102
103
52
53
53
54
55
55
56
95th
100
101
102
104
105
106
107
56
57
57
58
59
59
60
99th
108
108
109
111
112
113
114
64
64
65
65
66
67
67
50th
85
85
87
88
89
91
91
43
44
44
45
46
46
47
90th
98
99
100
101
103
104
105
57
58
58
59
60
61
61
95th
102
103
104
105
107
108
109
61
62
62
63
64
65
65
99th
109
110
111
112
114
115
116
69
69
70
70
71
72
72
50th
86
87
88
89
91
92
93
47
48
48
49
50
50
51
90th
100
100
102
103
104
106
106
61
62
62
63
64
64
65
95th
104
104
105
107
108
109
110
65
66
66
67
68
68
69
99th
111
111
113
114
115
116
117
73
73
74
74
75
76
76
50th
88
88
90
91
92
94
94
50
50
51
52
52
53
54
90th
101
102
103
104
106
107
108
64
64
65
66
67
67
68
95th
105
106
107
108
110
111
112
68
68
69
70
71
71
72
99th
112
113
114
115
117
118
119
76
76
76
77
78
79
79
50th
89
90
91
93
94
95
96
52
53
53
54
55
55
56
90th
103
103
105
106
107
109
109
66
67
67
68
69
69
70
95th
107
107
108
110
111
112
113
70
71
71
72
73
73
74
99th
114
114
116
117
118
120
120
78
78
79
79
80
81
81
50th
91
92
93
94
96
97
98
54
54
55
56
56
57
58
90th
104
105
106
108
109
110
111
68
68
69
70
70
71
72
95th
108
109
110
111
113
114
115
72
72
73
74
74
75
76
99th
115
116
117
119
120
121
122
80
80
80
81
82
83
83
50th
93
93
95
96
97
99
99
55
56
56
57
58
58
59
90th
106
107
108
109
111
112
113
69
70
70
71
72
72
73
95th
110
111
112
113
115
116
116
73
74
74
75
76
76
77
99th
117
118
119
120
122
123
124
81
81
82
82
83
84
84
50th
95
95
96
98
99
100
101
57
57
57
58
59
60
60
90th
108
109
110
111
113
114
114
71
71
71
72
73
74
74
95th
112
112
114
115
116
118
118
75
75
75
76
77
78
78
99th
119
120
121
122
123
125
125
82
82
83
83
84
85
86
50th
96
97
98
100
101
102
103
58
58
58
59
60
61
61
90th
110
110
112
113
114
116
116
72
72
72
73
74
75
75
95th
114
114
115
117
118
119
120
76
76
76
77
78
79
79
99th
121
121
123
124
125
127
127
83
83
84
84
85
86
87
50th
98
99
100
102
103
104
105
59
59
59
60
61
62
62
90th
112
112
114
115
116
118
118
73
73
73
74
75
76
76
95th
116
116
117
119
120
121
122
77
77
77
78
79
80
80
99th
123
123
125
126
127
129
129
84
84
85
86
86
87
88
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Age
(Year)
11
12
13
14
15
16
17
Systolic BP (mmHg)
Diastolic BP (mmHg)
← Percentile of Height →
← Percentile of Height →
BP
Percentile
↓
5th
10th
25th
50th
75th
90th
95th
5th
10th
25th
50th
75th
90th
95th
50th
100
101
102
103
105
106
107
60
60
60
61
62
63
63
90th
114
114
116
117
118
119
120
74
74
74
75
76
77
77
95th
118
118
119
121
122
123
124
78
78
78
79
80
81
81
99th
125
125
126
128
129
130
131
85
85
86
87
87
88
89
50th
102
103
104
105
107
108
109
61
61
61
62
63
64
64
90th
116
116
117
119
120
121
122
75
75
75
76
77
78
78
95th
119
120
121
123
124
125
126
79
79
79
80
81
82
82
99th
127
127
128
130
131
132
133
86
86
87
88
88
89
90
50th
104
105
106
107
109
110
110
62
62
62
63
64
65
65
90th
117
118
119
121
122
123
124
76
76
76
77
78
79
79
95th
121
122
123
124
126
127
128
80
80
80
81
82
83
83
99th
128
129
130
132
133
134
135
87
87
88
89
89
90
91
50th
106
106
107
109
110
111
112
63
63
63
64
65
66
66
90th
119
120
121
122
124
125
125
77
77
77
78
79
80
80
95th
123
123
125
126
127
129
129
81
81
81
82
83
84
84
99th
130
131
132
133
135
136
136
88
88
89
90
90
91
92
50th
107
108
109
110
111
113
113
64
64
64
65
66
67
67
90th
120
121
122
123
125
126
127
78
78
78
79
80
81
81
95th
124
125
126
127
129
130
131
82
82
82
83
84
85
85
99th
131
132
133
134
136
137
138
89
89
90
91
91
92
93
50th
108
108
110
111
112
114
114
64
64
65
66
66
67
68
90th
121
122
123
124
126
127
128
78
78
79
80
81
81
82
95th
125
126
127
128
130
131
132
82
82
83
84
85
85
86
99th
132
133
134
135
137
138
139
90
90
90
91
92
93
93
50th
108
109
110
111
113
114
115
64
65
65
66
67
67
68
90th
122
122
123
125
126
127
128
78
79
79
80
81
81
82
95th
125
126
127
129
130
131
132
82
83
83
84
85
85
86
99th
133
133
134
136
137
138
139
90
90
91
91
92
93
93
BP, blood pressure
* The 90th percentile is 1.28 SD, 95th percentile is 1.645 SD, and the 99th percentile is 2.326 SD over the mean. For research purposes,
the standard deviations in appendix table B–1 allow one to compute BP Z-scores and percentiles for girls with height percentiles given in
table 4 (i.e., the 5th, 10th, 25th, 50th, 75th, 90th, and 95th percentiles). These height percentiles must be converted to height Z-scores
given by (5% = -1.645; 10% = -1.28; 25% = -0.68; 50% = 0; 75% = 0.68; 90% = 1.28; 95% = 1.645) and then computed according to
the methodology in steps 2–4 described in appendix B. For children with height percentiles other than these, follow steps 1–4 as
described in appendix B.
Blood Pressure Tables
13
TABLE
5
Classification of Hypertension in Children and Adolescents,
With Measurement Frequency and Therapy Recommendations
SBP or DBP
Percentile*
Frequency of BP
Measurement
Therapeutic
Lifestyle Changes
Pharmacologic
Therapy
Normal
<90th
Recheck at next
scheduled physical
examination.
Encourage healthy —
diet, sleep, and
physical activity.
Prehypertension
90th to <95th
or if BP exceeds
120/80 mmHg
even if below 90th
percentile up to
<95th percentile†
Recheck in 6
months.
Weight-management counseling
if overweight,
introduce physical
activity and diet
management.‡
None unless
compelling
indications such
as CKD, diabetes
mellitus, heart failure, or LVH exist
Stage 1
hypertension
95th percentile to
the 99th percentile
plus 5 mmHg
Recheck in 1–2
weeks or sooner
if the patient is
symptomatic;
if persistently
elevated on two
additional occasions, evaluate
or refer to source
of care within
1 month.
Weight-management counseling
if overweight,
introduce physical
activity and diet
management.‡
Initiate therapy
based on indications in Table 6
or if compelling
indications as
above.
Stage 2
hypertension
>99th percentile
plus 5 mmHg
Evaluate or refer
to source of care
within 1 week
or immediately
if the patient is
symptomatic.
Weight-management counseling
if overweight,
introduce physical
activity and diet
management.‡
Initiate therapy.§
BP, blood pressure; CKD, chronic kidney disease; DBP, diastolic blood pressure; LVH, left ventricular hypertrophy; SBP,
systolic blood pressure
* For sex, age, and height measured on at least three separate occasions; if systolic and diastolic categories are different,
categorize by the higher value.
†
This occurs typically at 12 years old for SBP and at 16 years old for DBP.
‡
Parents and children trying to modify the eating plan to the Dietary Approaches to Stop Hypertension (DASH) eating plan
could benefit from consultation with a registered or licensed nutritionist to get them started.
§
More than one drug may be required.
TABLE
6
Indications for Antihypertensive Drug
Therapy in Children
■ Symptomatic hypertension
■ Secondary hypertension
■ Hypertensive target-organ damage
■ Diabetes (types 1 and 2)
■ Persistent hypertension despite
nonpharmacologic measures
14
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
TABLE
7
Clinical Evaluation of Confirmed Hypertension
Study or Procedure
Purpose
Target Population
History, including sleep history, family history, risk factors, diet, and habits such as
smoking and drinking alcohol; physical
examination
History and physical examination help
focus subsequent evaluation
All children with persistent BP ≥95th
percentile
BUN, creatinine, electrolytes, urinalysis,
and urine culture
R/O renal disease and chronic pyelonephritis All children with persistent BP ≥95th
percentile
CBC
R/O anemia, consistent with chronic renal
disease
All children with persistent BP ≥95th
percentile
Renal U/S
R/O renal scar, congenital anomaly, or
disparate renal size
All children with persistent BP ≥95th
percentile
Fasting lipid panel, fasting glucose
Identify hyperlipidemia, identify metabolic
abnormalities
Overweight patients with BP at 90th–94th
percentile; all patients with BP ≥95th
percentile. Family history of hypertension
or cardiovascular disease. Child with
chronic renal disease
Drug screen
Identify substances that might cause
hypertension
History suggestive of possible contribution
by substances or drugs
Polysomnography
Identify sleep disorder in association with
hypertension
History of loud, frequent snoring
Echocardiogram
Identify LVH and other indications of
cardiac involvement
Patients with comorbid risk factors* and BP
90th–94th percentile; all patients with BP
≥95th percentile
Retinal exam
Identify retinal vascular changes
Patients with comorbid risk factors* and BP
90th–94th percentile; all patients with BP
≥95th percentile
Ambulatory BP monitoring
Identify white-coat hypertension,
abnormal diurnal BP pattern, BP load
Patients in whom white-coat hypertension is
suspected, and when other information on
BP pattern is needed
Plasma renin determination
Identify low renin, suggesting mineralocorticoid-related disease
Young children with Stage 1 hypertension
and any child or adolescent with Stage 2
hypertension
Renovascular imaging
• Isotopic scintigraphy (renal scan)
• Magnetic resonance angiography
• Duplex Doppler flow studies
• 3-Dimensional CT
• Arteriography: DSA or classic
Identify renovascular disease
Young children with Stage 1 hypertension
and any child or adolescent with Stage 2
hypertension
Plasma and urine steroid levels
Identify steroid-mediated hypertension
Young children with Stage 1 hypertension
and any child or adolescent with Stage 2
hypertension
Plasma and urine catecholamines
Identify catecholamine-mediated hypertension Young children with Stage 1 hypertension
and any child or adolescent with Stage 2
hypertension
Evaluation for identifiable causes
Evaluation for comorbidity
Evaluation for target-organ damage
Further evaluation as indicated
Positive family history of severe hypertension
BP, blood pressure; BUN, blood urea nitrogen; CBC, complete blood count; CT, computerized tomography; DSA, digital subtraction angiography;
LVH, left ventricular hypertrophy; R/O, rule out; U/S, ultrasound
* Comorbid risk factors also include diabetes mellitus and kidney disease.
Blood Pressure Tables
15
Primary Hypertension
and Evaluation for Comorbidities
■
■
■
■
Primary hypertension is identifiable in children and adolescents.
Both hypertension and prehypertension have become a significant health issue
in the young due to the strong association of high BP with overweight and the
marked increase in the prevalence of overweight children.
The evaluation of hypertensive children should include assessment for additional
risk factors.
Due to an association of sleep apnea with overweight and high BP, a sleep history
should be obtained.
High BP in childhood had been considered
a risk factor for hypertension in early adulthood. However, primary (essential)
hypertension is now identifiable in children
and adolescents. Primary hypertension in
childhood is usually characterized by mild
or Stage 1 hypertension and is often associated with a positive family history of
hypertension or cardiovascular disease (CVD).
Children and adolescents with primary hypertension are frequently overweight. Data on
healthy adolescents obtained in school healthscreening programs demonstrate that the
prevalence of hypertension increases progressively with increasing body mass index (BMI),
and hypertension is detectable in approximately 30 percent of overweight children
(BMI >95th percentile).26 The strong association of high BP with obesity and the marked
increase in the prevalence of childhood obesity27 indicate that both hypertension and
prehypertension are becoming a significant
health issue in the young. Overweight children
frequently have some degree of insulin resistance—a prediabetic condition. Overweight
and high BP are also components of the
insulin-resistance syndrome or metabolic syndrome, a condition of multiple metabolic risk
factors for CVD as well as for type 2
diabetes.28,29 The clustering of other CVD
risk factors that are included in the insulinresistance syndrome (high triglycerides, low
16
high-density lipoprotein cholesterol [HDL-C],
truncal obesity, hyperinsulinemia) is significantly greater among children with high BP
than in children with normal BP.30 Recent
reports from studies that examined childhood
data estimate that the insulin-resistance syndrome is present in 30 percent of overweight
children with BMI greater than the 95th
percentile.31 Historically, hypertension in
childhood was considered a simple independent risk factor for CVD, but its link to
the other risk factors in the insulin-resistance
syndrome indicates that a broader approach
is more appropriate in affected children.
Primary hypertension often clusters with other
risk factors.31,32 Therefore, the medical history, physical examination, and laboratory
evaluation of hypertensive children and adolescents should include a comprehensive
assessment for additional cardiovascular risk.
These risk factors, in addition to high BP and
overweight, include low plasma HDL-C,
elevated plasma triglyceride, and abnormal
glucose tolerance. Fasting plasma insulin
concentration is generally elevated, but an elevated insulin concentration may be reflective
only of obesity and is not diagnostic of the
insulin-resistance syndrome. To identify other
cardiovascular risk factors, a fasting lipid
panel and fasting glucose level should be
obtained in children who are overweight and
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
have BP between the 90th and 94th percentile
and in all children with BP greater than the
95th percentile. If there is a strong family history of type 2 diabetes, a hemoglobin A1c or
glucose tolerance test may also be considered.
These metabolic risk factors should be
repeated periodically to detect changes in the
level of cardiovascular risk over time. Fewer
data are available on the utility of other tests
in children (e.g., plasma uric acid, or homocysteine and lp(a) levels), and the use of these
measures should depend on family history.
Sleep disorders, including sleep apnea, are
associated with hypertension, coronary artery
disease, heart failure, and stroke in adults.33,34
Although limited data are available, they suggest an association of sleep-disordered
breathing and higher BP in children.35,36
Approximately 15 percent of children snore,
and at least 1–3 percent have sleep-disordered
breathing.35 Because of the associations with
hypertension and the frequency of occurrence
of sleep disorders, particularly among
overweight children, a history of sleeping
patterns should be obtained in a child with
hypertension. One practical strategy for
identifying children with a sleep problem or
sleep disorder is to obtain a brief sleep history,
using an instrument called BEARS.37(table 1.1)
BEARS addresses five major sleep domains
that provide a simple but comprehensive
screen for the major sleep disorders affecting
children ages 2–18. The components of
BEARS include: Bedtime problems, Excessive
daytime sleepiness, Awakenings during the
night, Regularity and duration of sleep, and
Sleep-disordered breathing (snoring). Each
of these domains has an age-appropriate
trigger question and includes responses of
both parent and child, as appropriate. This
brief screening for sleep history can be completed in about 5 minutes.
In a child with primary hypertension, the presence of any comorbidity that is associated with
hypertension carries the potential to increase
the risk for CVD and can have an adverse
effect on health outcome. Consideration of
these associated risk factors and appropriate
evaluation in those children in whom the
hypertension is verified are important in planning and implementing therapies that reduce
the comorbidity risk as well as control BP.
Primary Hypertension and Evaluation for Comorbidities
17
Evaluation for Secondary Hypertension
■
■
■
■
Secondary hypertension is more common in children than in adults.
Because overweight is strongly linked to hypertension, BMI should be calculated
as part of the physical examination.
Once hypertension is confirmed, BP should be measured in both arms and in a leg.
Very young children, children with Stage 2 hypertension, and children or adolescents
with clinical signs that suggest systemic conditions associated with hypertension
should be evaluated more completely than in those with Stage 1 hypertension.
Secondary hypertension is more common in
children than in adults. The possibility that
some underlying disorder may be the cause of
the hypertension should be considered in
every child or adolescent who has elevated BP.
However, the extent of an evaluation for
detection of a possible underlying cause
should be individualized for each child. Very
young children, children with Stage 2 hypertension, and children or adolescents with
clinical signs that suggest the presence of systemic conditions associated with hypertension
should be evaluated more extensively as compared to those with Stage 1 hypertension.38
Present technologies may facilitate less invasive evaluation than in the past, although
experience in using newer modalities with
children is still limited.
A thorough history and physical examination
are the first steps in the evaluation of any
child with persistently elevated BP. Elicited
information should aim to identify not only
signs and symptoms due to high BP but also
clinical findings that might uncover an underlying systemic disorder. Thus, it is important
to seek signs and symptoms suggesting renal
disease (gross hematuria, edema, fatigue),
heart disease (chest pain, exertional dyspnea,
palpitations), and diseases of other organ systems (e.g., endocrinologic, rheumatologic).
Past medical history should elicit information
to focus the subsequent evaluation and to
18
uncover definable causes of hypertension.
Questions should be asked about prior hospitalizations, trauma, urinary tract infections,
snoring and other sleep problems. Questions
should address family history of hypertension,
diabetes, obesity, sleep apnea, renal disease,
other CVD (hyperlipidemia, stroke), and
familial endocrinopathies. Many drugs can
increase BP, so it is important to inquire
directly about use of over-the-counter, prescription, and illicit drugs. Equally important
are specific questions aimed at identifying the
use of nutritional supplements, especially
preparations aimed at enhancing athletic performance.
P H Y S I C A L E X A M I N AT I O N
The child’s height, weight, and percentiles for
age should be determined at the start of the
physical examination. Because obesity is
strongly linked to hypertension, BMI should
be calculated from the height and weight, and
the BMI percentile should be calculated. Poor
growth may indicate an underlying chronic
illness. When hypertension is confirmed, BP
should be measured in both arms and in a leg.
Normally, BP is 10–20 mmHg higher in the
legs than the arms. If the leg BP is lower than
the arm BP, or if femoral pulses are weak
or absent, coarctation of the aorta may be
present. Obesity alone is an insufficient explanation for diminished femoral pulses in the
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
presence of high BP. The remainder of the
physical examination should pursue clues
found on history and should focus on findings
that may indicate the cause and severity of
hypertension. Table 8 lists important physical
exam findings in hypertensive children.39
The physical examination in hypertensive
children is frequently normal except for the
BP elevation. The extent of the laboratory
evaluation is based on the child’s age, history,
physical examination findings, and level of BP
elevation. The majority of children with
secondary hypertension will have renal or
renovascular causes for the BP elevation.
Therefore, screening tests are designed to have
a high likelihood of detecting children and
adolescents who are so affected. These tests
are easily obtained in most primary care
offices and community hospitals. Additional
evaluation must be tailored to the specific
child and situation. The risk factors, or
comorbid conditions, associated with primary
hypertension should be included in the evaluation of hypertension in all children, as well
as efforts to determine any evidence of targetorgan damage.
ADDITIONAL DIAGNOSTIC
STUDIES FOR
HYPERTENSION
Additional diagnostic studies may be appropriate in the evaluation of hypertension in a
child or adolescent, particularly if there is a
high degree of suspicion that an underlying
disorder is present. Such procedures are listed
in table 7. ABPM, discussed previously, has
application in evaluating both primary and
secondary hypertension. ABPM is also used
to detect white-coat hypertension.
RENIN PROFILING
Plasma renin level or plasma renin activity
(PRA) is a useful screening test for mineralocorticoid-related diseases. With these
disorders, the PRA is very low or unmeasurable by the laboratory and may be associated
with relative hypokalemia. PRA levels are
higher in patients who have renal artery
stenosis. However, approximately 15 percent
of children with arteriographically evident
renal artery stenosis have normal PRA
values.40–42 Assays for direct measurement
of renin, a different technique than PRA, are
commonly used, although extensive normative data in children and adolescents are
unavailable.
E VA L U AT I O N F O R P O S S I B L E
R E N O VA S C U L A R
HYPERTENSION
Renovascular hypertension is a consequence
of an arterial lesion or lesions impeding blood
flow to one or both kidneys or to one or
more intrarenal segments.43,44 Affected children usually, but not invariably, have
markedly elevated BP.40,44 Evaluation for renovascular disease also should be considered in
infants or children with other known predisposing factors, such as prior umbilical artery
catheter placements or neurofibromatosis.44,45
A number of newer diagnostic techniques are
presently available for evaluation of renovascular disease, but experience in their use in
pediatric patients is limited. Consequently, the
recommended approaches generally use older
techniques, such as standard intra-arterial
angiography, digital-subtraction angiography
(DSA), and scintigraphy (with or without
angiotensin-converting enzyme [ACE] inhibition).44 As technologies evolve, children
should be referred for imaging studies to centers that have expertise in the radiological
evaluation of childhood hypertension.
I N VA S I V E S T U D I E S
Intra-arterial DSA with contrast is used more
frequently than standard angiography, but,
because of intra-arterial injection, this method
remains invasive. DSA also can be accomplished by using a rapid injection of contrast
into a peripheral vein, but quality of views
and the size of pediatric veins make this technique useful only for older children. DSA and
formal arteriography are still considered the
“gold standard,” but these studies should be
undertaken only when surgical or invasive
interventional radiologic techniques are being
contemplated for anatomic correction.46
Evaluation for Secondary Hypertension
19
TABLE
8
Examples of Physical Examination Findings Suggestive of Definable Hypertension *
Vital signs
Finding†
Possible Etiology
Tachycardia
Hyperthyroidism, pheochromocytoma,
neuroblastoma, primary hypertension
Coarctation of the aorta
Decreased lower
extremity pulses;
drop in BP from upper
to lower extremities
Eyes
Retinal changes
Severe hypertension, more likely to be associated
with secondary hypertension
Ear, nose, and throat
(ENT)
Adenotonsillar
hypertrophy
Suggests association with sleep-disordered
breathing (sleep apnea), snoring
Height/weight
Growth retardation
Obesity (high BMI)
Truncal obesity
Chronic renal failure
Primary hypertension
Cushing syndrome, insulin resistance syndrome
Head and neck
Moon facies
Elfin facies
Webbed neck
Thyromegaly
Cushing syndrome
Williams syndrome
Turner syndrome
Hyperthyroidism
Skin
Pallor, flushing,
diaphoresis
Acne, hirsutism, striae
Café-au-lait spots
Adenoma sebaceum
Malar rash
Acanthrosis nigricans
Pheochromocytoma
Widely spaced nipples
Heart murmur
Friction rub
Turner syndrome
Coarctation of the aorta
Systemic lupus erythematosus (pericarditis),
collagen-vascular disease, end stage renal disease
with uremia
Left ventricular hypertrophy/chronic hypertension
Chest
Apical heave
Cushing syndrome, anabolic steroid abuse
Neurofibromatosis
Tuberous sclerosis
Systemic lupus erythematosus
Type 2 diabetes
Abdomen
Mass
Epigastric/flank bruit
Palpable kidneys
Wilms tumor, neuroblastoma, pheochromocytoma
Renal artery stenosis
Polycystic kidney disease, hydronephrosis, multicystic-dysplastic kidney, mass (see above)
Genitalia
Ambiguous/virilization
Adrenal hyperplasia
Extremities
Joint swelling
Systemic lupus erythematosus, collagen vascular
disease
Muscle weakness
Hyperaldosteronism, Liddle syndrome
BMI, body mass index; BP, blood pressure
* Adapted from Flynn, JT. Evaluation and management of hypertension in childhood. Prog Pediatr Cardiol 2001;12:177–88.
†
20
Findings listed are examples of physical findings and do not represent all possible physical findings.
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Newer imaging techniques may be used in
children with vascular lesions. Magnetic
resonance angiography (MRA) is increasingly
feasible for the evaluation of pediatric
renovascular disease, but it is still best for
detecting abnormalities in the main renal
artery and its primary branches.47–49 Imaging
with magnetic resonance requires that the
patient be relatively immobile for extended
periods—a significant difficulty for small children. At present, studies are needed to assess
the effectiveness of MRA in the diagnosis of
children with renovascular disease. Newer
methods, including 3-dimensional (3-D)
reconstructions of computerized tomography
(CT) images, or spiral CT with contrast,
appear promising in evaluating children who
may have renovascular disease.50
Evaluation for Secondary Hypertension
21
Target-Organ Abnormalities
in Childhood Hypertension
■
■
■
■
Target-organ abnormalities are commonly associated with hypertension in children
and adolescents.
Left ventricular hypertrophy (LVH) is the most prominent evidence of target-organ
damage.
Pediatric patients with established hypertension should have echocardiographic
assessment of left ventricular mass at diagnosis and periodically thereafter.
The presence of LVH is an indication to initiate or intensify antihypertensive
therapy.
Hypertension is associated with increased risk
of myocardial infarction, stroke, and cardiovascular mortality in adults,2,51 and treatment
of elevated BP results in a reduction in the
risk for cardiovascular events.
Children and adolescents with severe elevation
of BP are also at increased risk of adverse outcomes, including hypertensive encephalopathy,
seizures, and even cerebrovascular accidents
and congestive heart failure.52,53 Even hypertension that is less severe contributes to
target-organ damage when it occurs with
other chronic conditions, such as chronic
kidney disease.54–56 Two autopsy studies,57,58
that evaluated tissue from adolescents and
young adults who had sudden deaths due to
trauma, demonstrated significant relationships
between the level of BP, or hypertension, and
the presence of atherosclerotic lesions in the
aorta and coronary arteries. The exact level
and duration of BP elevation that causes
target-organ damage in the young has not
been established.
One difficulty in the assessment of these
relationships is that, until recently, few noninvasive methods could evaluate the effect of
hypertension on the cardiovascular system.
Noninvasive techniques that use ultrasound
can demonstrate structural and functional
changes in the vasculature related to BP.
22
Recent clinical studies using these techniques
demonstrate that childhood levels of BP are
associated with carotid intimal-medial thickness59 and large artery compliance60 in young
adults. Even healthy adolescents with clustering of cardiovascular risk factors
demonstrate elevated carotid thickness,61,62
and those with BP levels at the higher end of
the normal distribution show decreased
brachial artery flow-mediated vasodilatation.
Overall, evidence is increasing that even mild
BP elevation can have an adverse effect on
vascular structure and function63 in asymptomatic young persons.
LVH is the most prominent clinical evidence of
target-organ damage caused by hypertension
in children and adolescents. With the use of
echocardiography to measure left ventricular
mass, LVH has been reported in 34–38 percent of children and adolescents with mild,
untreated BP elevation.64–66 Daniels et al. evaluated 130 children and adolescents with
persistent BP elevation.67 They reported that
55 percent of patients had a left ventricular
mass index greater than the 90th percentile,
and 14 percent had left ventricular mass index
above 51 g/m2.7, a value in adults with hypertension that has been associated with a
fourfold greater risk of adverse cardiovascular
outcomes. When left ventricular geometry
was examined in hypertensive children,
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
17 percent had concentric hypertrophy, a pattern that is associated with higher risk for
cardiovascular outcomes in adults, and
30 percent had eccentric hypertrophy, which
is associated with intermediate risk for cardiovascular outcomes.67
In addition, abnormalities of the retinal vasculature have been reported in adults with
hypertension.68 Few studies of retinal abnormalities have been conducted in children with
hypertension. Skalina et al. evaluated newborns with hypertension69 and reported the
presence of hypertensive retinal abnormalities
in approximately 50 percent of their patients.
On repeat examination, after the resolution of
hypertension, these abnormalities had disappeared.
C L I N I C A L R E C O M M E N D AT I O N
Echocardiography is recommended as a
primary tool for evaluating patients for targetorgan abnormalities by assessing the presence
or absence of LVH. Left ventricular mass is
determined from standard echocardiographic
measurements of the left ventricular end-diastolic dimension (LVED), the intraventricular
septal thickness (IVS), and the thickness of the
left ventricular posterior wall (LVPW) and can
be calculated as: LV Mass (g) = 0.80 [1.04
(IVS + LVED + LVPW)3 – (LVED)3] + 0.6
(with echocardiographic measurements in centimeters). From these measures, the left
ventricular mass can be calculated by using
the equation of Devereux et al.70 when measurements are made according to the criteria of
the American Society of Echocardiography.71
Heart size is closely associated with body
size.72 Left ventricular mass index is calculated to standardize measurements of left
ventricular mass. Several methods for
indexing left ventricular mass have been
reported, but it is recommended that height
(m2.7) be used to index left ventricular mass,
as described by de Simone et al.73 This
method accounts for close to the equivalent of
the effect of lean body mass and excludes the
effect of obesity and BP elevation on left ventricular mass. Some echo laboratories use
height as the indexing variable. This calculation is also acceptable and is somewhat easier
to use, as fewer calculations are needed.
Children and adolescents with established
hypertension should have an echocardiogram
to determine if LVH is present. A conservative cutpoint that determines the presence of
LVH is 51 g/m2.7. This cutpoint is above the
99th percentile for children and adolescents
and is associated with increased morbidity in
adults with hypertension.73 Other references
exist for normal children,74 but, unlike adults,
outcome-based standards for left ventricular
mass index are not available for children. In
interpreting the left ventricular mass index, it
should be remembered that some factors, such
as obesity and hypertension, have pathologic
effects on the heart, whereas others—such as
physical activity, particularly in highly conditioned athletes—may be adaptive.
Ascertainment of left ventricular mass index
is very helpful in clinical decisionmaking.
The presence of LVH can be an indication for
initiating or intensifying pharmacologic
therapy to lower BP. For patients who have
LVH, the echocardiographic determination of
left ventricular mass index should be repeated
periodically.
At the present time, additional testing for other
target-organ abnormalities (such as determination of carotid intimal-medial thickness and
evaluation of urine for microalbuminuria) is
not recommended for routine clinical use.
Further research will be needed to evaluate the
clinical utility of these tests.
Target-Organ Abnormalities in Childhood Hypertension
23
Therapeutic
Lifestyle Changes
■
■
■
■
Weight reduction is the primary therapy for obesity-related hypertension.
Prevention of excess or abnormal weight gain will limit future increases in BP.
Regular physical activity and restriction of sedentary activity will improve efforts
at weight management and may prevent an excess increase in BP over time.
Dietary modification should be strongly encouraged in children and adolescents who
have BP levels in the prehypertensive range as well as in those with hypertension.
Family-based intervention improves success.
Evidence is limited that supports the efficacy
of nonpharmacological interventions for BP
reduction in the treatment of hypertension in
children and adolescents. Data that demonstrate a relationship of lifestyle with BP can be
used as the basis for recommendations. On
the basis of large randomized controlled trials,
the following lifestyle modifications are recommended in adults:2 weight reduction in
overweight or obese individuals;75 increased
intake of fresh vegetables, fruits, and lowfat
dairy (the Dietary Approaches to Stop
Hypertension Study [DASH] eating plan);76
dietary sodium reduction;76,77 increased physical activity;78 and moderation of alcohol
consumption.79 Smoking cessation has significant cardiovascular benefits.32 As information
on chronic sleep problems evolves, interventions to improve sleep quality may also have a
beneficial effect on BP.80
The potential for control of BP in children
through weight reduction is supported by BP
tracking and weight-reduction studies. BP
levels track from childhood through adolescence and into adulthood81–83 in association
with weight.84,85 Because of the strong correlation between weight and BP, excessive
weight gain is likely to be associated with elevated BP over time. Therefore, maintenance
of normal weight gain in childhood should
lead to less hypertension in adulthood.
24
Weight loss in overweight adolescents is associated with a decrease in BP.30,86–90 Weight
control not only decreases BP, it also
decreases BP sensitivity to salt88 and decreases
other cardiovascular risk factors, such as dyslipidemia and insulin resistance.32 In studies
that achieve a reduction in BMI of about
10 percent, short-term reductions in BP were
in the range of 8–12 mmHg. Although difficult, weight loss, if successful, is extremely
effective.32,91–93 Identifying a complication of
overweight, such as hypertension, can be a
helpful motivator for patients and families to
make changes. Weight control can render
pharmacological treatment unnecessary but
should not delay drug use when indicated.
Emphasis on the management of complications rather than on overweight shifts the aim
of weight management from an aesthetic to a
health goal. In motivated families, education
or simple behavior modification can be successful in achieving moderate weight loss or
preventing further weight gain. Steps can be
implemented in the primary care setting even
with limited staff and time resources.32,91 The
patient should be encouraged to self-monitor
time spent in sedentary activity, including
watching television and playing video or computer games, and to set goals to progressively
decrease these activities to less than 2 hours
per day.94 The family and patient should
identify physical activities that the child enjoys,
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
engage in them regularly, and self-monitor time
spent in physical activities (30–60 minutes per
day should be achieved).94–96 Dietary changes
can involve portion-size control, decrease in
consumption of sugar-containing beverages and
energy-dense snacks, increase in consumption
of fresh fruits and vegetables, and regular
meals including a healthy breakfast.32,91,93,97,98
Consultation with a nutritionist can be useful
and provide customized recommendations.
During regular office visits, the primary care
provider can supervise the child’s progress in
self-monitoring and accomplishing goals and
can provide support and positive feedback to
the family. Some patients will benefit from a
more intense and comprehensive approach to
weight management from a multidisciplinary
and specialized team if available.91–93
Despite the lack of firm evidence about
dietary intervention in children, it is generally
accepted that hypertensive individuals can
benefit from a dietary increase in fresh vegetables, fresh fruits, fiber, and nonfat dairy, as
well as a reduction of sodium. Despite some
suggestion that calcium supplements may
decrease BP in children,99,100 so far the evidence is too limited to support a clinical
recommendation.101 Lower BP has been associated in children and adolescents with an
increased intake of potassium,100–103 magnesium,100,101 folic acid,101,104 unsaturated
fat,100,105,106 and fiber,100,101,104 and lower
dietary intake of total fat.100,101 However,
these associations are small and insufficient to
support dietary recommendations for specific,
individual nutrients.
Sodium reduction in children and adolescents
has been associated with small reductions in
BP, in the range of 1–3 mmHg.101,103,107–110
Data from one randomized trial suggest that
sodium intake in infancy may affect BP in
adolescence.111 Similarly, some evidence indicates that breastfeeding may be associated
with lower BP in childhood.112,113 The current
recommendation for adequate daily sodium
intake is only 1.2 g/day for 4- to 8-year-old
children and 1.5 g/day for older children.114
Since this amount of sodium is substantially
lower than current dietary intakes, lowering
dietary sodium from the current usual intake
may have future benefit. Reduced sodium
intake, with calorie restriction, may account
for some of the BP improvement associated
with weight loss.
Regular physical activity has cardiovascular
benefits. A recent meta-analysis that combined 12 randomized trials, for a total of
1,266 children and adolescents, concluded
that physical activity leads to a small, but not
statistically significant, decrease in BP.115
However, both regular physical activity and
decreasing sedentary activity—such as
watching television and playing video or electronic games—are important components of
pediatric obesity treatment and prevention.32,91–93 Weight-reduction trials
consistently report better results when physical activity and/or prevention of sedentary
activity are included in the treatment protocol. Therefore, regular aerobic physical
activity (30–60 minutes of moderate physical
activity on most days) and limitation of
sedentary activities to less than 2 hours per
day are recommended for the prevention of
obesity, hypertension, and other cardiovascular risk factors.94–96 With the exception of
power lifting, resistance training is also
helpful. Competitive sports participation
should be limited only in the presence of
uncontrolled Stage 2 hypertension.116
The scope of hypertension as a public health
problem in adults is substantial. Poor healthrelated behaviors such as physical inactivity,
unfavorable dietary patterns, and excessive
weight gain raise the risk for future hypertension. The therapeutic lifestyle changes
discussed above may have benefit for all children in prevention of future disease, including
primary hypertension. Accordingly, appropriate health recommendations for all children
and adolescents are regular physical activity; a
diet with limited sodium but rich in fresh
fruits, fresh vegetables, fiber, and lowfat dairy;
and avoiding excess weight gain.
Therapeutic Lifestyle Changes
25
Pharmacologic Therapy
of Childhood Hypertension
■
■
■
■
■
Indications for antihypertensive drug therapy in children include secondary
hypertension and insufficient response to lifestyle modifications.
Recent clinical trials have expanded the number of drugs that have pediatric dosing
information. Dosing recommendations for many of the newer drugs are provided.
Pharmacologic therapy, when indicated, should be initiated with a single drug.
Acceptable drug classes for use in children include ACE inhibitors, angiotensinreceptor blockers, beta-blockers, calcium channel blockers, and diuretics.
The goal for antihypertensive treatment in children should be reduction of BP
to <95th percentile, unless concurrent conditions are present. In that case,
BP should be lowered to <90th percentile.
Severe, symptomatic hypertension should be treated with intravenous
antihypertensive drugs.
In adults, hypertension is typically a lifelong
condition. Most hypertensive patients will
need to remain on medications for the rest of
their lives. Usually, adults readily accept this
fact, given the known long-term adverse consequences of untreated or undertreated
hypertension.117 In children, however, the
long-term consequences of untreated hypertension are unknown. Additionally, no data are
available on the long-term effects of antihypertensive drugs on growth and development.
Therefore, a definite indication for initiating
pharmacologic therapy should be ascertained
before a drug is prescribed.
Table 6 summarizes the indications for use of
antihypertensive drugs in children. These
indications include symptomatic hypertension,
secondary hypertension, established hypertensive target-organ damage, and failure of
nonpharmacologic measures. Other indications for use of antihypertensive drugs can be
considered, depending on the clinical situation. For example, because the presence of
multiple cardiovascular risk factors (elevated
BP, dyslipidemia, tobacco use, etc.) increases
cardiovascular risk in an exponential rather
26
than additive fashion,118,119 antihypertensive
therapy could be considered if the child or
adolescent is known to have dyslipidemia.
The number of antihypertensive drugs has
increased since the publication of the Report
of the Task Force on Blood Pressure Control
in Children.120 The number of drugs that
have been studied systematically in children
has also increased, largely because of incentives provided to the pharmaceutical industry
under the auspices of the 1997 Food and
Drug Administration Modernization Act
(FDAMA) and the 2002 Best Pharmaceuticals
for Children Act (BPCA).121–123 These developments have had both negative and positive
consequences. Chief among the negative consequences is the lack of reliable pediatric data
for older, commonly used compounds with
expired patent protection. Currently, no
incentives exist for industry-sponsored trials
of such drugs, and alternative methods of
stimulating pediatric studies, such as those
contained in the BPCA,123–125 have yet to
come to fruition. On the other hand, publication of the results of industry-sponsored
clinical trials and single-center case series will
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
provide additional data that can be combined
with prior recommendations based on expert
opinion and collective clinical experience to
guide the use of antihypertensive drugs in
children and adolescents who require pharmacologic treatment.
blockers or calcium channel blockers in hypertensive children with migraine headaches.
This approach is similar to that outlined in
the recent JNC 7 report, which recommends
specific classes of antihypertensive drugs for
use in adults in certain high-risk categories.2
Table 9 contains dosing recommendations for
antihypertensive drugs in children 1–17 years
old. It should be noted that many other drugs
are available in addition to those listed in table
9. Those drugs are not included in the table,
however, because few or no pediatric data were
available at the time this report was prepared.
All antihypertensive drugs should be prescribed in a similar fashion: The child is
initially started on the lowest recommended
dose listed in table 9. The dose can be
increased until the desired BP goal is achieved.
Once the highest recommended dose is
reached, or if the child experiences side effects
from the drug, a second drug from a different
class should be added. Consideration should
be given to combining drugs with complementary mechanisms of action, such as an
ACE inhibitor with a diuretic, or a vasodilator
with a diuretic or beta-adrenergic blocker.
Because little pediatric experience is available
in using fixed-dose combination products,
except for bisoprolol/HCTZ,131 routine use of
these products in children cannot be recommended at this time.
Long-term, clinical endpoint data from randomized trials, such as the Antihypertensive
and Lipid-Lowering Treatment to Prevent
Heart Attack Trial (ALLHAT), support the
preferential use of specific antihypertensive
drugs in adults.2,126 However, pediatric clinical trials of antihypertensive drugs have
focused only on their ability to lower BP and
have not compared the effects of these drugs
on clinical endpoints. Therefore, because all
classes of antihypertensive drugs have been
shown to lower BP in children, the choice of
drug for initial antihypertensive therapy
resides in the preference of the responsible
physician. Some diuretics and beta-adrenergic
blockers, which were recommended as initial
therapy in the first and second Task Force
Reports,25,120 have a long history of safety
and efficacy based on clinical experience in
hypertensive children, and these drugs remain
appropriate for pediatric use. Similarly, some
members of the newer classes of antihypertensive drugs, including ACE inhibitors, calcium
channel blockers, and angiotensin-receptor
blockers,127–130 have been studied in children
and, based on short-term use, shown to be
safe and well-tolerated with satisfactory BP
reductions in hypertensive children.
Specific classes of antihypertensive drugs
should be used preferentially in certain hypertensive children with specific underlying or
concurrent medical conditions. Examples
include the use of ACE inhibitors or
angiotensin-receptor blockers in children with
diabetes and microalbuminuria or proteinuric
renal diseases, and the use of beta-adrenergic
For children with uncomplicated primary
hypertension and no hypertensive targetorgan damage, the goal BP should be less
than the 95th percentile for sex, age, and
height, whereas for children with chronic
renal disease, diabetes, or hypertensive targetorgan damage, the goal BP should be less
than the 90th percentile for sex, age, and
height. Again, this approach is similar to the
recommended treatment of hypertension in
adults with additional cardiovascular risk
factors or comorbid conditions.2
Important adjunctive aspects to the drug
therapy of childhood hypertension include
ongoing monitoring of target-organ damage as
well as BP monitoring, surveillance for drug
side effects, periodic monitoring of electrolytes
in children treated with ACE inhibitors or
diuretics, counseling regarding other cardiovascular risk factors, and continued emphasis
on nonpharmacologic measures. It may also
be appropriate to consider “step-down”
therapy in selected patients. This approach
attempts a gradual reduction in the drug after
an extended course of good BP control, with
Pharmacologic Therapy of Childhood Hypertension
27
TABLE
9
Antihypertensive Drugs for Outpatient Management of Hypertension in Children 1–17 Years Old*
Class
Drug
Dose†
Angiotensin-converting
enzyme (ACE) inhibitor
Benazepril
Initial: 0.2 mg/kg/day up to 10 mg/day
Maximum: 0.6 mg/kg/day up to 40 mg/day
Captopril
Initial: 0.3–0.5 mg/kg/dose
Maximum: 6 mg/kg/day
Enalapril
Initial: 0.08 mg/kg/day up to 5 mg/day
Maximum: 0.6 mg/kg/day up to 40 mg/day
Fosinopril
Children >50 kg:
Initial: 5–10 mg/day
Maximum: 40 mg/day
Lisinopril
Initial: 0.07 mg/kg/day up to 5 mg/day
Maximum: 0.6 mg/kg/day up to 40 mg/day
Quinapril
Initial: 5–10 mg/day
Maximum: 80 mg/day
Irbesartan
6–12 years: 75–150 mg/day
≥13 years: 150–300 mg/day
Losartan
Initial: 0.7 mg/kg/day up to 50 mg/day
Maximum: 1.4 mg/kg/day up to 100 mg/day
α- and β-blocker
Labetalol
Initial: 1–3 mg/kg/day
Maximum: 10–12 mg/kg/day up to 1,200 mg/day
β-blocker
Atenolol
Initial: 0.5–1 mg/kg/day
Maximum: 2 mg/kg/day up to 100 mg/day
Bisoprolol/HCTZ
Initial: 2.5/6.25 mg/day
Maximum: 10/6.25 mg/day
Metoprolol
Initial: 1–2 mg/kg/day
Maximum: 6 mg/kg/day up to 200 mg/day
Propranolol
Initial: 1–2 mg/kg/day
Maximum: 4 mg/kg/day up to 640 mg/day
Amlodipine
Children 6–17 years:
2.5–5 mg once daily
Felodipine
Initial: 2.5 mg/day
Maximum: 10 mg/day
Isradipine
Initial: 0.15–0.2 mg/kg/day
Maximum: 0.8 mg/kg/day up to 20 mg/day
Extended-release
nifedipine
Initial: 0.25–0.5 mg/kg/day
Maximum: 3 mg/kg/day up to 120 mg/day
Angiotensin-receptor blocker
Calcium channel blocker
28
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Dosing Interval
Evidence‡
FDA Labelings§ Comments††
qd
RCT
Yes
1. All ACE inhibitors are contraindicated in pregnancy—females of
childbearing age should use reliable contraception.
tid
RCT, CS
No
2. Check serum potassium and creatinine periodically to monitor for
hyperkalemia and azotemia.
qd–bid
RCT
Yes
3. Cough and angioedema are reportedly less common with newer members
of this class than with captopril.
qd
RCT
Yes
4. Benazepril, enalapril, and lisinopril labels contain information on the
preparation of a suspension; captopril may also be compounded into a
suspension.
qd
RCT
Yes
qd
RCT, EO
No
5. FDA approval for ACE inhibitors with pediatric labeling is limited to
children ≥6 years of age and to children with creatinine clearance
≥30 ml/min/1.73m2.
qd
CS
Yes
1. All ARBs are contraindicated in pregnancy—females of childbearing age
should use reliable contraception.
qd
RCT
Yes
2. Check serum potassium, creatinine periodically to monitor for
hyperkalemia and azotemia.
3. Losartan label contains information on the preparation of a suspension.
4. FDA approval for ARBs is limited to children ≥6 years of age and to
children with creatinine clearance ≥30 ml/min/1.73m2.
bid
CS, EO
No
1. Asthma and overt heart failure are contraindications.
2. Heart rate is dose-limiting.
3. May impair athletic performance.
4. Should not be used in insulin-dependent diabetics.
qd–bid
CS
No
1. Noncardioselective agents (propranolol) are contraindicated in asthma
and heart failure.
qd
RCT
No
2. Heart rate is dose-limiting.
bid
CS
No
bid–tid
RCT, EO
Yes
qd
RCT
Yes
1. Amlodipine and isradipine can be compounded into stable extemporaneous suspensions.
qd
RCT, EO
No
2. Felodipine and extended-release nifedipine tablets must be swallowed
whole.
tid–qid
CS, EO
No
3. Isradipine is available in both immediate-release and sustained-release
formulations; sustained release form is dosed qd or bid.
qd–bid
CS, EO
No
4. May cause tachycardia.
3. May impair athletic performance.
4. Should not be used in insulin-dependent diabetics.
5. A sustained-release formulation of propranolol is available that is dosed
once-daily.
Pharmacologic Therapy of Childhood Hypertension
29
TABLE
9
Antihypertensive Drugs for Outpatient Management of Hypertension in Children 1–17 Years Old*
(continued)
Class
Drug
Dose†
Central α-agonist
Clonidine
Children ≥12 years:
Initial: 0.2 mg/day
Maximum: 2.4 mg/day
Diuretic
HCTZ
Initial: 1 mg/kg/day
Maximum: 3 mg/kg/day up to 50 mg/day
Chlorthalidone
Initial: 0.3 mg/kg/day
Maximum: 2 mg/kg/day up to 50 mg/day
Furosemide
Initial: 0.5–2.0 mg/kg/dose
Maximum: 6 mg/kg/day
Spironolactone
Initial: 1 mg/kg/day
Maximum: 3.3 mg/kg/day up to 100 mg/day
Triamterene
Initial: 1–2 mg/kg/day
Maximum: 3–4 mg/kg/day up to 300 mg/day
Amiloride
Initial: 0.4–0.625 mg/kg/day
Maximum: 20 mg/day
Doxazosin
Initial: 1 mg/day
Maximum: 4 mg/day
Prazosin
Initial: 0.05–0.1 mg/kg/day
Maximum: 0.5 mg/kg/day
Terazosin
Initial: 1 mg/day
Maximum: 20 mg/day
Hydralazine
Initial: 0.75 mg/kg/day
Maximum: 7.5 mg/kg/day up to 200 mg/day
Minoxidil
Children <12 years:
Initial: 0.2 mg/kg/day
Maximum: 50 mg/day
Children ≥12 years:
Initial: 5 mg/day
Maximum: 100 mg/day
Peripheral α-antagonist
Vasodilator
30
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Dosing Interval
Evidence‡
bid
EO
FDA Labelings§ Comments††
Yes
1. May cause dry mouth and/or sedation.
2. Transdermal preparation also available.
3. Sudden cessation of therapy can lead to severe rebound hypertension.
qd
EO
Yes
1. All patients treated with diuretics should have electrolytes monitored
shortly after initiating therapy and periodically thereafter.
qd
EO
No
2. Useful as add-on therapy in patients being treated with drugs from other
drug classes.
qd–bid
EO
No
3. Potassium-sparing diuretics (spironolactone, triamterene, amiloride) may
cause severe hyperkalemia, especially if given with ACE inhibitor or ARB.
qd–bid
EO
No
bid
EO
No
4. Furosemide is labeled only for treatment of edema but may be useful as
add-on therapy in children with resistant hypertension, particularly in
children with renal disease.
qd
EO
No
qd
EO
No
tid
EO
No
qd
EO
No
qid
EO
Yes
qd–tid
CS, EO
Yes
5. Chlorthalidone may precipitate azotemia in patients with renal diseases
and should be used with caution in those with severe renal impairment.
1. May cause hypotension and syncope, especially after first dose.
1. Tachycardia and fluid retention are common side effects.
2. Hydralazine can cause a lupus-like syndrome in slow acetylators.
3. Prolonged use of minoxidil can cause hypertrichosis.
4. Minoxidil is usually reserved for patients with hypertension resistant
to multiple drugs.
ACE, angiotensin-converting enzyme; ARB, angiotensin-receptor blocker; bid, twice-daily; HCTZ, hydrochlorothiazide; qd, once-daily; qid, four times daily; tid,
three times daily
* Includes drugs with prior pediatric experience or recently completed clinical trials.
† The maximum recommended adult dose should not be exceeded in routine clinical practice.
‡ Level of evidence upon which dosing recommendations are based (CS, case series; EO, expert opinion; RCT, randomized controlled trial)
§ FDA-approved pediatric labeling information is available. Recommended doses for agents with FDA-approved pediatric labels are the doses contained in
the approved labels. Even when pediatric labeling information is not available, the FDA-approved label should be consulted for additional safety information.
†† Comments apply to all members of each drug class except where otherwise stated.
Pharmacologic Therapy of Childhood Hypertension
31
FIGURE
1
Management Algorithm
Measure BP and Height and Calculate BMI
Determine BP category for sex, age, and height*
Stage 2 Hypertension*
Stage 1 Hypertension*
Repeat BP
Prehypertensive*
90–<95%
Over 3 visits
or 120/80 mmHg
≥95%
Therapeutic
Lifestyle
Changes†
Normotensive*
<90%
90–<95% or 120/80 mmHg
Diagnostic Workup
Include Evaluation for
Target-Organ Damage‡
Diagnostic Workup
Include Evaluation for
Target-Organ Damage‡
Secondary
or Primary
Hypertension Hypertension
Secondary
Hypertension
Consider Referral
Rx Specific
for Cause
To provider with expertise in
pediatric hypertension
Normal
BMI
Drug Rx
≥95%
Overweight
Weight Reduction
and Drug Rx
Drug Rx‡
For the Family
Repeat BP
In 6 months
or Primary
Hypertension
Consider Diagnostic Workup
and Evaluation for TargetOrgan Damage‡
Therapeutic
Lifestyle
Changes†
If overweight or comorbidity exists
Normal Overweight
BMI
Still ≥95%
Educate on
Heart Health
Lifestyle†
Normal
BMI
Weight Reduction Monitor Q 6 Mo
Overweight
Weight Reduction
BMI, body mass index; BP, blood pressure; Rx, prescription; Q, every.
*See tables 3, 4, and 5.
†Diet
modification and physical activity.
‡Especially
32
if younger, very high BP, little or no family history, diabetic, or other risk factors.
the eventual goal of completely discontinuing
drug therapy. Children with uncomplicated
primary hypertension, especially overweight
children who successfully lose weight, are the
best candidates for the step-down approach.
Such patients require ongoing BP monitoring
after the cessation of drug therapy, as well as
continued nonpharmacologic treatment,
because hypertension may recur.
hours.132,133 Hypertensive urgencies are
accompanied by less serious symptoms, such
as severe headache or vomiting. Hypertensive
urgencies can be treated by either intravenous
or oral antihypertensives, depending on the
child’s symptomatology. Table 10 provides
dosing recommendations for treatment of
severe hypertension in children when prompt
reduction in BP is indicated.
Severe, symptomatic hypertension with BP
well above the 99th percentile occurs in some
children, usually those with underlying renal
disease, and requires prompt treatment.
Hypertensive emergencies in children are usually accompanied by signs of hypertensive
encephalopathy, typically causing seizures.
Hypertensive emergencies should be treated
by an intravenous antihypertensive that can
produce a controlled reduction in BP, aiming
to decrease the pressure by 25 percent or less
over the first 8 hours after presentation and
then gradually normalizing the BP over 26–48
Figure 1 is a management algorithm that presents guidelines for evaluation and treatment
of Stage 1 and Stage 2 hypertension in children and adolescents. The algorithm
summarizes monitoring and intervention recommendations for children and adolescents
with prehypertension and hypertension.
Included in the algorithm are points at which
the presence of overweight is considered in
clinical decisionmaking. The algorithm also
emphasizes the inclusion of evaluation for
target-organ damage in children with established Stage 1 and Stage 2 hypertension.
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
TABLE
10
Antihypertensive Drugs for Management of Severe Hypertension
in Children 1–17 Years Old
Most Useful*
Drug
Class
Dose†
Route
Comments
Esmolol
ß-blocker
100–500 mcg/kg/min
iv infusion
Very short-acting—constant
infusion preferred. May
cause profound bradycardia.
Produced modest reductions
in BP in a pediatric clinical
trial.
Hydralazine
Vasodilator
0.2–0.6 mg/kg/dose
iv, im
Should be given every 4 hours
when given iv bolus.
Recommended dose is lower
than FDA label.
Labetalol
α- and ßblocker
bolus: 0.2–1.0
mg/kg/dose up to 40
mg/dose
infusion: 0.25–3.0
mg/kg/hr
iv bolus or
infusion
Asthma and overt heart
failure are relative contraindications.
Nicardipine
Calcium
channel
blocker
1–3 mcg/kg/min
iv infusion
May cause reflex tachycardia.
Sodium
nitroprusside
Vasodilator
0.53–10 mcg/kg/min
iv infusion
Monitor cyanide levels with
prolonged (>72 hr) use or in
renal failure; or coadminister
with sodium thiosulfate.
Occasionally Useful‡
Drug
Class
Dose*
Route
Comments
Clonidine
Central
α-agonist
0.05–0.1 mg/dose
may be repeated up
to 0.8 mg total dose
po
Side effects include dry
mouth and sedation.
Enalaprilat
ACE inhibitor
0.05–0.1 mg/kg/dose
up to 1.25 mg/dose
iv bolus
May cause prolonged
hypotension and acute renal
failure, especially in neonates.
Fenoldopam
Dopamine
receptor
agonist
0.2–0.8 mcg/kg/min
iv infusion
Produced modest reductions
in BP in a pediatric clinical
trial in patients up to 12
years.
Isradipine
Calcium chan- 0.05–0.1 mg/kg/dose
nel blocker
po
Stable suspension can be
compounded.
Minoxidil
Vasodilator
po
Most potent oral vasodilator;
long-acting.
0.1–0.2 mg/kg/dose
ACE, angiotensin-converting enzyme; im, intramuscular; iv, intravenous; po, oral.
* Useful for hypertensive emergencies and some hypertensive urgencies.
† All dosing recommendations are based upon expert opinion or case series data except as otherwise noted.
‡ Useful for hypertensive urgencies and some hypertensive emergencies.
Pharmacologic Therapy of Childhood Hypertension
33
APPENDIX A.
Demographic Data
34
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Appendix A. Demographic Data
35
A–1
(49)
31,066
(29)
18,022
605
(10)
6,288
988
1,830
(54)
34,409
437
1,324
11,311
(3)
1,764
0
64
1,677
(1)
654
0
10
644
(3)
1,972
74
12
1,800
2
(0)
118
0
32
0
0
* Table differs from 1997 report: updated height percentile used; subjects whose height Z-score was less than –6 or greater than +6 were excluded.
DBP.5, diastolic blood pressure (Korotkoff 5); NHANES, National Health and Nutrition Examination Survey; NIH, National Institutes of Health; SBP, systolic blood pressure.
of Total)
(51)
32,161
1,063
1,770
555
0
6,368
83,091
57,976
47,500
2,076
2,076
4,304
5,042
2,104
4,304
19,207
5,042
19,409
560
19,207
898
19,409
371
6,368
461
63,227
(Percent
1–17
1,041
2,577
3,422
0
Total
8–17
NHANES
2,465
9,418
431
0
6,430
2,104
5–17
NHANES III
9,991
4
0
0
0
0
2,834
2,834
99–00
9–17
Minnesota
24
0
0
85
0
0
7,358
15,882
11,565
21,852
11,565
21,860
0
0
285
893
3,609
3,609
3,647
3,647
0
231
0
0
0
0
0
1
0
Missing
4,092
230
4,092
0
0
0
0
0
84
Other
1–3
0
3,320
23
0
0
0
0
Native
American
Providence
0
0
748
0
0
0
0
Asian
0
1,993
3,110
1,341
4,878
4,729
176
2,963
White
4,092
2,099
3,263
637
0
1,570
0
0
Hispanic
5–17
3,167
1,377
2,480
5,266
108
600
Black
Person’s
Visits
DBP.5
Available
Iowa
4–17
South
1,457
3,607
5,649
137
1,751
Girls
Person’s
Visits
SBP
Available
6,430
3–17
Houston
3,751
5,916
148
1,896
Boys
Ethnic Group
Carolina
1–17
Bogalusa
1–5
Pittsburgh
13–17
6–17
NIH
Dallas
(Years)
Age
Source
Gender
Demographic Data on Height/Blood Pressure Distribution Curves by Study Population*
TABLE
83,091
63,227
2,104
2,104
5,042
5,042
19,409
19,409
898
461
4,092
4,092
6,430
6,430
2,834
2,834
15,882
7,358
21,860
11,565
893
285
3,647
3,647
Total
No. of
Person’s
Visits
APPENDIX B.
Computation of Blood Pressure
Percentiles for Arbitrary Sex, Age,
and Height
36
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Computation of Blood Pressure
Percentiles for Arbitrary Sex, Age,
and Height
■
To compute the systolic blood pressure (SBP) percentile of a boy who is age y years
and height h inches with SBP = x mmHg:
1. Refer to the most recent CDC growth charts, which are available online, and convert the
height of h inches to a height Z-score relative to boys of the same age; this is denoted by Zht.
2. Compute the expected SBP (µ) for boys of age y years and height h inches given by
4
4
µ = α + Σ β j (y-10) + Σ γ k (Zht)
j=1
j
k
k=1
where α, β 1…, β4 and γ1…, γ4 are given in the 3rd column of appendix table B–1.
3. Then convert the boy’s observed SBP to a Z-score (Zbp) given by
Zbp = (x – µ)/σ
where σ is given in the 3rd column of appendix table B–1.
4. To convert the bp Z-score to a percentile (P), compute P = Φ (Zbp) x 100%
where Φ (Z) = area under a standard normal distribution to the left of Z.
Thus, if Zbp = 1.28, then Φ (Zbp) = .90 and the bp percentile = .90 x 100% = 90%.
5. To compute percentiles for SBP for girls, diastolic blood pressure (DBP) (K5) for boys,
and DBP (K5) for girls, use the regression coefficients from the 4th, 5th, and 6th columns
of appendix table B–1.
For example, a 12-year-old boy, with height at the 90th percentile for his age-sex group,
has a height Z-score = 1.28, and his expected SBP (µ) is
µ = 102.19768 + 1.82416 (2) + 0.12776 (22) + 0.00249 (23) –0.00135 (24) + 2.73157
(1.28) –0.19618 (1.28)2 –0.04659 (1.28)3 + 0.00947 (1.28)4 = 109.46 mmHg.
Suppose his actual SBP is 120 mmHg (x); his SBP Z-score is then:
SBP Z-score = (x – µ)/σ = (120–109.46)/10.7128 = 0.984
The corresponding SBP percentile = Φ (0.984) x 100% = 83.7th percentile.
Appendix B. Computation of Blood Pressure Percentiles for Arbitrary Sex, Age, and Height
37
TABLE
B–1
Regression Coefficients From Blood Pressure Regression Models*
Systolic BP
Variable Name
Diastolic BP5
Symbol
Male
Female
Male
Female
α
102.19768
102.01027
61.01217
60.50510
Age–10
β1
1.82416
1.94397
0.68314
1.01301
(Age–10)2
β2
0.12776
0.00598
-0.09835
0.01157
Intercept
Age
(Age–10)3
β3
0.00249
-0.00789
0.01711
0.00424
(Age–10)4
β4
-0.00135
-0.00059
0.00045
-0.00137
Normalized height
Zht
γ1
2.73157
2.03526
1.46993
1.16641
Zht2
γ2
-0.19618
0.02534
-0.07849
0.12795
Zht3
γ3
-0.04659
-0.01884
-0.03144
-0.03869
Zht4
γ4
0.00947
0.00121
0.00967
-0.00079
Standard deviation
ρ†
n (persons)
n (visits)
σ
10.4855
11.6032
0.4100
0.3824
0.2436
0.2598
32,161
31,066
24,057
23,443
42,074
41,017
29,182
28,794
10.7128
10.9573
BP, blood pressure; Diastolic BP5, diastolic measurement at Korotkoff 5.
* The coefficients were obtained from mixed-effects linear regression models.
† The value of ρ represents the correlation between BP measurements at different ages for the same child after correcting for age
and Zht. This computation was necessary because some studies contributing to the childhood BP database provided BP at more
than one age.
38
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
Scheme Used for
Classification of the Evidence
M
Meta-analysis; use of statistical
methods to combine the results from
clinical trials
RA Randomized controlled trials;
also known as experimental studies
RE Retrospective analyses; also known
as case-control studies
F
Prospective study; also known as cohort
studies, including historical
or prospective followup studies
X
Cross-sectional survey; also known
as prevalence studies
PR
Previous review or position
statements
C
Clinical interventions
(nonrandomized)
These symbols are appended to the citations
in the reference list. The studies that provided
evidence supporting the recommendations
of this report were classified and reviewed
by the staff and the executive committee.
The classification scheme is from the JNC 7
report and other NHBPEP Working Group
Reports (www.nhlbi.nih.gov/about/nhbpep/
index.htm).2,134–138
Scheme Used for Classification of the Evidence
39
References
1.
2.
3.
Chobanian AV, Bakris GL, Black HR,
Cushman WC, Green LA, Izzo JL, Jr., et al.
The Seventh Report of the Joint National
Committee on Prevention, Detection,
Evaluation, and Treatment of High Blood
Pressure: The JNC 7 report. JAMA
2003;289:2560–72. PR
Prineas RJ, Jacobs D. Quality of Korotkoff
sounds: Bell vs diaphragm, cubital fossa vs
brachial artery. Prev Med 1983;12:715–9.
4.
Londe S, Klitzner TS. Auscultatory blood
pressure measurement—effect of pressure on
the head of the stethoscope. West J Med
1984;141:193–5.
5.
Prineas RJ. Blood pressure in children and
adolescents. In: Bulpitt CJ, ed. Epidemiology
of hypertension. New York: Elsevier; 2000,
86–105. Birkenhager WH and Reid JL, eds.
Handbook of hypertension, v. 20.
6.
7.
40
National High Blood Pressure Education
Program Working Group on Hypertension
Control in Children and Adolescents. Update
on the 1987 Task Force Report on High
Blood Pressure in Children and Adolescents:
A working group report from the National
High Blood Pressure Education Program.
Pediatrics 1996;98:649–58. PR
Mourad A, Carney S, Gillies A, Jones B,
Nanra R, Trevillian P. Arm position and
blood pressure: A risk factor for hypertension? J Hum Hypertens 2003;17:389–95.
Netea RT, Lenders JW, Smits P, Thien T.
Both body and arm position significantly
influence blood pressure measurement.
J Hum Hypertens 2003;17:459–62.
8.
Rocchini AP. Coarctation of the aorta and
interrupted aortic arch. In: Moller JH,
Hoffmann U, eds. Pediatric cardiovascular
medicine. New York: Churchill Livingstone;
2000, p. 570.
9.
Gomez-Marin O, Prineas RJ, Rastam L. Cuff
bladder width and blood pressure measurement in children and adolescents. J Hypertens
1992;10:1235–41.
10. American Heart Association. Home monitoring of high blood pressure. Available at:
www.americanheart.org/presenter.jhtml?identifier=576. Verified July 12, 2004.
11. Prineas RJ. Measurement of blood pressure
in the obese. Ann Epidemiol
1991;1:321–36. PR
12. Ostchega Y, Prineas RJ, Paulose-Ram R,
Grim CM, Willard G, Collins D. National
Health and Nutrition Examination Survey
1999–2000: Effect of observer training and
protocol standardization on reducing blood
pressure measurement error. J Clin
Epidemiol 2003;56:768–74.
13. Lewington S, Clarke R, Qizilbash N, Peto R,
Collins R. Age-specific relevance of usual
blood pressure to vascular mortality: A
meta-analysis of individual data for one million adults in 61 prospective studies. Lancet
2002;360:1903–13. M
14. Jones DW, Appel LJ, Sheps SG, Roccella EJ,
Lenfant C. Measuring blood pressure accurately: New and persistent challenges. JAMA
2003;289:1027–30. PR
15. Canzanello VJ, Jensen PL, Schwartz GL. Are
aneroid sphygmomanometers accurate in
hospital and clinic settings? Arch Intern
Med 2001;161:729–31. PR
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
16. Butani L, Morgenstern BZ. Are pitfalls of
oxcillometric blood pressure measurements
preventable in children? Pediatr Nephrol
2003;18:313–8. PR
17. Kaufmann MA, Pargger H, Drop LJ.
Oscillometric blood pressure measurements
by different devices are not interchangeable.
Anesth Analg 1996;82:377–81.
18. Park MK, Menard SW, Yuan C. Comparison
of auscultatory and oscillometric blood pressures. Arch Pediatr Adolesc Med
2001;155:50–3. RA
19. O'Brien E, Pickering T, Asmar R, Myers M,
Parati G, Staessen J, et al. Working Group
on Blood Pressure Monitoring of the
European Society of Hypertension
International Protocol for validation of blood
pressure measuring devices in adults. Blood
Press Monit 2002;7:3–17. PR
20. O'Brien E, Coats A, Owens P, Petrie J,
Padfield PL, Littler WA, et al. Use and
interpretation of ambulatory blood
pressure monitoring: Recommendations
of the British hypertension society. BMJ
2000;320:1128–34. PR
21. Sorof JM, Portman RJ. Ambulatory blood
pressure measurements. Curr Opin Pediatr
2001;13:133–7.
22. Simckes AM, Srivastava T, Alon US.
Ambulatory blood pressure monitoring in
children and adolescents. Clin Pediatr (Phila)
2002;41:549–64. PR
23. Lurbe E, Sorof JM, Daniels SR. Clinical and
research aspects of ambulatory blood pressure monitoring in children. J Pediatr
2004;144:7–16. PR
25. Task Force on Blood Pressure Control in
Children. Report of the Second Task Force
on Blood Pressure Control in Children—
1987. National Heart, Lung, and Blood
Institute, Bethesda, Maryland. Pediatrics
1987;79:1–25. PR
26. Sorof J, Daniels S. Obesity hypertension
in children: A problem of epidemic proportions. Hypertension 2002;40:441–7. PR
27. Ogden CL, Flegal KM, Carroll MD, Johnson
CL. Prevalence and trends in overweight
among US children and adolescents,
1999–2000. JAMA 2002;288:1728–32. X
28. Reaven GM. Insulin resistance/compensatory
hyperinsulinemia, essential hypertension, and
cardiovascular disease. J Clin Endocrinol
Metab 2003;88:2399–403.
29. U.S. Department of Health and Human
Services, National Institutes of Health,
National Heart, Lung, and Blood Insitute,
National Cholesterol Education Program.
Third Report of the Expert Panel on
Detection, Evaluation, and Treatment of
High Blood Cholesterol in Adults (Adult
Treatment Panel III) final report. NIH
Publication No. 02-5215. Bethesda, MD:
National Heart, Lung, and Blood Institute.
September 2002. PR
30. Sinaiko AR, Steinberger J, Moran A, Prineas
RJ, Jacobs DR, Jr. Relation of insulin resistance to blood pressure in childhood. J
Hypertens 2002;20:509–17. RA
31. Cook S, Weitzman M, Auinger P, Nguyen M,
Dietz WH. Prevalence of a metabolic syndrome phenotype in adolescents: Findings
from the third National Health and Nutrition
Examination Survey, 1988–1994. Arch
Pediatr Adolesc Med 2003;157:821–7. X
24. Centers for Disease Control and Prevention,
National Center for Health Statistics. 2000
CDC Growth Charts: United States.
Available at: www.cdc.gov/growthcharts/.
Verified July 12, 2004.
References
41
32. Williams CL, Hayman LL, Daniels SR,
Robinson TN, Steinberger J, Paridon S, et al.
Cardiovascular health in childhood: A statement for health professionals from the
Committee on Atherosclerosis, Hypertension,
and Obesity in the Young (AHOY) of the
Council on Cardiovascular Disease in the
Young, American Heart Association.
Circulation 2002;106:143–60. PR
33. Quan SF, Gersh BJ. Cardiovascular consequences of sleep-disordered breathing: Past,
present and future: Report of a workshop
from the National Center on Sleep Disorders
Research and the National Heart, Lung, and
Blood Institute. Circulation 2004;109:951–7.
34. Strohl KP. Invited commentary: To sleep,
perchance to discover. Am J Epidemiol
2002;155:394–5.
35. Marcus CL, Greene MG, Carroll JL. Blood
pressure in children with obstructive sleep
apnea. Am J Respir Crit Care Med
1998;157:1098–103. X
36. Enright PL, Goodwin JL, Sherrill DL, Quan
JR, Quan SF. Blood pressure elevation associated with sleep-related breathing disorder in
a community sample of white and Hispanic
children: The Tucson Children's Assessment
of Sleep Apnea study. Arch Pediatr Adolesc
Med 2003;157:901–4. F
37. Mindell JA, Owens JA. A clinical guide to
pediatric sleep: Diagnosis and management
of sleep problems. Philadelphia, PA:
Lippincott Williams & Wilkins; 2003, p. 10,
Table 1.1.
38. Sinaiko AR. Hypertension in children.
N Engl J Med 1996;335:1968–73. PR
39. Flynn JT. Evaluation and management of
hypertension in childhood. Prog Pediatr
Cardiol 2001;12:177–88. PR
40. Hiner LB, Falkner B. Renovascular hypertension in children. Pediatr Clin North Am
1993;40:123–40. PR
42
41. Dillon MJ, Ryness JM. Plasma renin activity
and aldosterone concentration in children.
Br Med J 1975;4:316–9. X
42. Guzzetta PC, Potter BM, Ruley EJ, Majd M,
Bock GH. Renovascular hypertension in children: Current concepts in evaluation and
treatment. J Pediatr Surg 1989;24:1236–40. C
43. Watson AR, Balfe JW, Hardy BE.
Renovascular hypertension in childhood:
A changing perspective in management.
J Pediatr 1985;106:366–72.
44. Dillon MJ. The diagnosis of renovascular
disease. Pediatr Nephrol 1997;11:366–72. PR
45. Mena E, Bookstein JJ, Holt JF, Fry WJ.
Neurofibromatosis and renovascular hypertension in children. Am J Roentgenol
Radium Ther Nucl Med 1973;118:39–45. RE
46. Shahdadpuri J, Frank R, Gauthier BG, Siegel
DN, Trachtman H. Yield of renal arteriography in the evaluation of pediatric hypertension. Pediatr Nephrol 2000;14:816–9. RE
47. Binkert CA, Debatin JF, Schneider E, Hodler
J, Ruehm SG, Schmidt M, et al. Can MR
measurement of renal artery flow and renal
volume predict the outcome of percutaneous
transluminal renal angioplasty? Cardiovasc
Intervent Radiol 2001;24:233–9. F
48. Marcos HB, Choyke PL. Magnetic resonance
angiography of the kidney. Semin Nephrol
2000;20:450–5. PR
49. Debatin JF, Spritzer CE, Grist TM, Beam C,
Svetkey LP, Newman GE, et al. Imaging of
the renal arteries: Value of MR angiography.
AJR Am J Roentgenol 1991;157:981–90. F
50. Vade A, Agrawal R, Lim-Dunham J, Hartoin
D. Utility of computed tomographic renal
angiogram in the management of childhood
hypertension. Pediatr Nephrol
2002;17:741–7. RE
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
51. MacMahon S, Peto R, Cutler J, Collins R,
Sorlie P, Neaton J, et al. Blood pressure,
stroke, and coronary heart disease. Part 1,
Prolonged differences in blood pressure:
Prospective observational studies corrected
for the regression dilution bias. Lancet
1990;335:765–74. F
52. Still JL, Cottom D. Severe hypertension in
childhood. Arch Dis Child 1967;42:34–9.
PR
53. Gill DG, Mendes de Costa B, Cameron JS,
Joseph MC, Ogg CS, Chantler C. Analysis
of 100 children with severe and persistent
hypertension. Arch Dis Child
1976;51:951–6. F
54. Johnstone LM, Jones CL, Grigg LE,
Wilkinson JL, Walker RG, Powell HR. Left
ventricular abnormalities in children, adolescents and young adults with renal disease.
Kidney Int 1996;50:998–1006. X
55. Mitsnefes MM, Daniels SR, Schwartz SM,
Khoury P, Strife CF. Changes in left ventricular mass in children and adolescents during
chronic dialysis. Pediatr Nephrol
2001;16:318–23. F
56. Mitsnefes MM, Kimball TR, Witt SA,
Glascock BJ, Khoury PR, Daniels SR. Left
ventricular mass and systolic performance in
pediatric patients with chronic renal failure.
Circulation 2003;107:864–8. X
57. Berenson GS, Srinivasan SR, Bao W,
Newman WP, III, Tracy RE, Wattigney WA.
Association between multiple cardiovascular
risk factors and atherosclerosis in children
and young adults. The Bogalusa Heart Study.
N Engl J Med 1998;338:1650–6. F
58. McGill HC, Jr., McMahan CA, Zieske AW,
Malcom GT, Tracy RE, Strong JP. Effects of
nonlipid risk factors on atherosclerosis in
youth with a favorable lipoprotein profile.
Circulation 2001;103:1546–50.
59. Davis PH, Dawson JD, Riley WA, Lauer RM.
Carotid intimal-medial thickness is related to
cardiovascular risk factors measured from
childhood through middle age: The
Muscatine Study. Circulation
2001;104:2815–9. F
60. Arnett DK, Glasser SP, McVeigh G, Prineas
R, Finklestein S, Donahue R, et al. Blood
pressure and arterial compliance in young
adults: The Minnesota Children's Blood
Pressure Study. Am J Hypertens
2001;14:200–5. F
61. Knoflach M, Kiechl S, Kind M, Said M, Sief
R, Gisinger M, et al. Cardiovascular risk factors and atherosclerosis in young males:
ARMY study (Atherosclerosis Risk-Factors in
Male Youngsters). Circulation
2003;108:1064–9. X
62. Sanchez A, Barth JD, Zhang L. The carotid
artery wall thickness in teenagers is related to
their diet and the typical risk factors of heart
disease among adults. Atherosclerosis
2000;152:265–6.
63. Barnes VA, Treiber FA, Davis H. Impact of
Transcendental Meditation on cardiovascular
function at rest and during acute stress in
adolescents with high normal blood pressure.
J Psychosom Res 2001;51:597–605. RA
64. Belsha CW, Wells TG, McNiece KL, Seib
PM, Plummer JK, Berry PL. Influence of
diurnal blood pressure variations on target
organ abnormalities in adolescents with mild
essential hypertension. Am J Hypertens
1998;11:410–7. F
65. Sorof JM, Alexandrov AV, Cardwell G,
Portman RJ. Carotid artery intimal-medial
thickness and left ventricular hypertrophy in
children with elevated blood pressure.
Pediatrics 2003;111:61–6.
References
43
66. Hanevold C, Waller J, Daniels S, Portman R,
Sorof J. The effects of obesity, gender, and
ethnic group on left ventricular hypertrophy
and geometry in hypertensive children: A
collaborative study of the International
Pediatric Hypertension Association.
Pediatrics 2004;113:328–33. X
73. de Simone G, Daniels SR, Devereux RB,
Meyer RA, Roman MJ, de Divitiis O, et al.
Left ventricular mass and body size in normotensive children and adults: Assessment
of allometric relations and impact of overweight. J Am Coll Cardiol
1992;20:1251–60. F
67. Daniels SR, Loggie JM, Khoury P, Kimball
TR. Left ventricular geometry and severe left
ventricular hypertrophy in children and
adolescents with essential hypertension.
Circulation 1998;97:1907–11. X
74. Daniels SR, Kimball TR, Morrison JA,
Khoury P, Meyer RA. Indexing left ventricular mass to account for differences in body
size in children and adolescents without cardiovascular disease. Am J Cardiol
1995;76:699–701. X
68. Svardsudd K, Wedel H, Aurell E, Tibblin G.
Hypertensive eye ground changes.
Prevalence, relation to blood pressure and
prognostic importance. The study of men
born in 1913. Acta Med Scand
1978;204:159–67. F
69. Skalina ME, Annable WL, Kliegman RM,
Fanaroff AA. Hypertensive retinopathy in
the newborn infant. J Pediatr
1983;103:781–6. X
70. Devereux RB, Alonso DR, Lutas EM,
Gottlieb GJ, Campo E, Sachs I, et al.
Echocardiographic assessment of left ventricular hypertrophy: Comparison to necropsy
findings. Am J Cardiol 1986;57:450–8. RE
71. Sahn DJ, DeMaria A, Kisslo J, Weyman A.
Recommendations regarding quantitation in
M-mode echocardiography: Results of a survey of echocardiographic measurements.
Circulation 1978;58:1072–83.
72. Daniels SR, Kimball TR, Morrison JA,
Khoury P, Witt S, Meyer RA. Effect of lean
body mass, fat mass, blood pressure, and sexual maturation on left ventricular mass in
children and adolescents. Statistical, biological, and clinical significance. Circulation
1995;92:3249–54. X
75. He J, Whelton PK, Appel LJ, Charleston J,
Klag MJ. Long-term effects of weight loss
and dietary sodium reduction on incidence of
hypertension. Hypertension 2000;35:544–9. F
76. Sacks FM, Svetkey LP, Vollmer WM, Appel
LJ, Bray GA, Harsha D, et al. Effects on
blood pressure of reduced dietary sodium and
the Dietary Approaches to Stop Hypertension
(DASH) diet. DASH-Sodium Collaborative
Research Group. N Engl J Med
2001;344:3–10. RA
77. Vollmer WM, Sacks FM, Ard J, Appel LJ,
Bray GA, Simons-Morton DG, et al. Effects
of diet and sodium intake on blood pressure:
Subgroup analysis of the DASH-sodium trial.
Ann Intern Med 2001;135:1019–28. RA
78. Whelton SP, Chin A, Xin X, He J. Effect of
aerobic exercise on blood pressure: A metaanalysis of randomized, controlled trials.
Ann Intern Med 2002;136:493–503. M
79. Xin X, He J, Frontini MG, Ogden LG,
Motsamai OI, Whelton PK. Effects of alcohol reduction on blood pressure: A metaanalysis of randomized controlled trials.
Hypertension 2001;38:1112–7. M
80. Ayas NT, White DP, Manson JE, Stampfer
MJ, Speizer FE, Malhotra A, et al. A
prospective study of sleep duration and coronary heart disease in women. Arch Intern
Med 2003;163:205–9. X
44
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
81. Cook NR, Gillman MW, Rosner BA, Taylor
JO, Hennekens CH. Combining annual
blood pressure measurements in childhood to
improve prediction of young adult blood
pressure. Stat Med 2000;19:2625–40. F
82. Lauer RM, Mahoney LT, Clarke WR.
Tracking of blood pressure during childhood:
The Muscatine Study. Clin Exp Hypertens A
1986;8:515–37. F
83. Lauer RM, Clarke WR. Childhood risk
factors for high adult blood pressure:
The Muscatine Study. Pediatrics
1989;84:633–41. F
84. Clarke WR, Woolson RF, Lauer RM.
Changes in ponderosity and blood pressure
in childhood: The Muscatine Study. Am J
Epidemiol 1986;124:195–206. F
85. Burke V, Beilin LJ, Dunbar D. Tracking of
blood pressure in Australian children.
J Hypertens 2001;19:1185–92. F
86. Figueroa-Colon R, Franklin FA, Lee JY, von
Almen TK, Suskind RM. Feasibility of a
clinic-based hypocaloric dietary intervention
implemented in a school setting for obese
children. Obes Res 1996;4:419–29. RA
87. Wabitsch M, Hauner H, Heinze E, Muche R,
Bockmann A, Parthon W, et al. Body-fat distribution and changes in the atherogenic riskfactor profile in obese adolescent girls during
weight reduction. Am J Clin Nutr
1994;60:54–60. C
88. Rocchini AP, Key J, Bondie D, Chico R,
Moorehead C, Katch V, et al. The effect of
weight loss on the sensitivity of blood pressure to sodium in obese adolescents. N Engl
J Med 1989;321:580–5. C
89. Rocchini AP, Katch V, Anderson J,
Hinderliter J, Becque D, Martin M, et al.
Blood pressure in obese adolescents: Effect
of weight loss. Pediatrics 1988;82:16–23.
RA
90. Sinaiko AR, Gomez-Marin O, Prineas RJ.
Relation of fasting insulin to blood pressure
and lipids in adolescents and parents.
Hypertension 1997;30:1554–9. X
91. Robinson TN. Behavioural treatment of
childhood and adolescent obesity. Int J Obes
Relat Metab Disord
1999;23 Suppl 2:S52–S57. PR
92. Epstein LH, Myers MD, Raynor HA, Saelens
BE. Treatment of pediatric obesity. Pediatrics
1998;101:554–70. PR
93. Barlow SE, Dietz WH. Obesity evaluation
and treatment: Expert Committee recommendations. The Maternal and Child Health
Bureau, Health Resources and Services
Administration and the Department of
Health and Human Services. Pediatrics
1998;102:e29. Available at:
www.pediatrics.org/cgi/content/full/102/3/e29.
Verified July 12, 2004. PR
94. Krebs NF, Jacobson MS. Prevention of pediatric overweight and obesity. Pediatrics
2003;112:424–30. PR
95. U.S. Department of Health and Human
Services. The Surgeon General's call to action
to prevent and decrease overweight and
obesity. Rockville, MD: U.S. Department
of Health and Human Services, Public Health
Service, Office of the Surgeon General. 2001.
PR
96. Gutin B, Owens S. Role of exercise intervention in improving body fat distribution and
risk profile in children. Am J Human Biol
1999;11:237–47. RA
97. Siega-Riz AM, Popkin BM, Carson T. Trends
in breakfast consumption for children in the
United States from 1965–1991. Am J Clin
Nutr 1998;67:748S–756S.
98. Warren JM, Henry CJ, Simonite V. Low
glycemic index breakfasts and reduced food
intake in preadolescent children. Pediatrics
2003;112:e414. Available at:
www.pediatrics.org/cgi/content/full/112/
5/e414. Verified July 12, 2004. RA
References
45
99. Gillman MW, Hood MY, Moore LL, Nguyen
US, Singer MR, Andon MB. Effect of calcium supplementation on blood pressure in
children. J Pediatr 1995;127:186–92. RA
100. Simons-Morton DG, Hunsberger SA, Van
Horn L, Barton BA, Robson AM, McMahon
RP, et al. Nutrient intake and blood pressure
in the Dietary Intervention Study in Children.
Hypertension 1997;29:930–6. RA
101. Simons-Morton DG, Obarzanek E. Diet and
blood pressure in children and adolescents.
Pediatr Nephrol 1997;11:244–9. PR
102. Miller JZ, Weinberger MH, Christian JC.
Blood pressure response to potassium supplementation in normotensive adults and children. Hypertension 1987;10:437–42. C
103. Sinaiko AR, Gomez-Marin O, Prineas RJ.
Effect of low sodium diet or potassium supplementation on adolescent blood pressure.
Hypertension 1993;21:989–94. RA
104. Falkner B, Sherif K, Michel S, Kushner H.
Dietary nutrients and blood pressure in
urban minority adolescents at risk for
hypertension. Arch Pediatr Adolesc Med
2000;154:918–22. X
105. Stern B, Heyden S, Miller D, Latham G,
Klimas A, Pilkington K. Intervention study
in high school students with elevated blood
pressures. Dietary experiment with polyunsaturated fatty acids. Nutr Metab
1980;24:137–47. C
106. Goldberg RJ, Ellison RC, Hosmer DW, Jr.,
Capper AL, Puleo E, Gamble WJ, et al.
Effects of alterations in fatty acid intake on
the blood pressure of adolescents: The
Exeter-Andover Project. Am J Clin Nutr
1992;56:71–6. F
107. Cooper R, Van Horn L, Liu K, Trevisan M,
Nanas S, Ueshima H, et al. A randomized
trial on the effect of decreased dietary sodium
intake on blood pressure in adolescents.
J Hypertens 1984;2:361–6. RA
46
108. Falkner B, Michel S. Blood pressure response
to sodium in children and adolescents. Am J
Clin Nutr 1997;65:618S–621S. PR
109. Gillum RF, Elmer PJ, Prineas RJ. Changing
sodium intake in children. The Minneapolis
Children's Blood Pressure Study.
Hypertension 1981;3:698–703. RA
110. Howe PR, Cobiac L, Smith RM. Lack of
effect of short-term changes in sodium intake
on blood pressure in adolescent schoolchildren. J Hypertens 1991;9:181–6. RA
111. Geleijnse JM, Hofman A, Witteman JC,
Hazebroek AA, Valkenburg HA, Grobbee
DE. Long-term effects of neonatal sodium
restriction on blood pressure. Hypertension
1997;29:913–7. RA
112. Martin RM, Ness AR, Gunnell D, Emmett P,
Smith GD. Does breast-feeding in infancy
lower blood pressure in childhood? The Avon
Longitudinal Study of Parents and Children
(ALSPAC). Circulation 2004;109:1259–66. F
113. Wilson AC, Forsyth JS, Greene SA, Irvine L,
Hau C, Howie PW. Relation of infant diet to
childhood health: Seven year follow up of
cohort of children in Dundee infant feeding
study. BMJ 1998;316:21–5. F
114. Panel of Dietary Intakes for Electrolytes and
Water, Standing Committee on the Scientific
Evaluation of Dietary Reference Intakes,
Food and Nutrition Board, Institute of
Medicine. Dietary reference intakes for
water, potassium, sodium, chloride, and
sulfate. Washington, DC: National
Academies Press. 2004. Available at:
www.nap.edu/books/0309091691/html/.
Verified July 12, 2004. PR
115. Kelley GA, Kelley KS, Tran ZV. The effects
of exercise on resting blood pressure in children and adolescents: A meta-analysis of
randomized controlled trials. Prev Cardiol
2003;6:8–16. M
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
116. American Academy of Pediatrics. American
Academy of Pediatrics Committee on Sports
Medicine and Fitness. Athletic participation
by children and adolescents who have systemic hypertension. Pediatrics
1997;99:637–8. PR
117. Klag MJ, Whelton PK, Randall BL, Neaton
JD, Brancati FL, Ford CE, et al. Blood pressure and end-stage renal disease in men.
N Engl J Med 1996;334:13–8. F
126. ALLHAT Officers and Coordinators for the
ALLHAT Collaborative Research Group.
Major outcomes in high-risk hypertensive
patients randomized to angiotensinconverting enzyme inhibitor or calcium channel blocker vs diuretic: The Antihypertensive
and Lipid-Lowering Treatment to Prevent
Heart Attack Trial (ALLHAT). JAMA
2002;288:2981–97. RA
118. Yusuf HR, Giles WH, Croft JB, Anda RF,
Casper ML. Impact of multiple risk factor
profiles on determining cardiovascular
disease risk. Prev Med 1998;27:1–9. X
127. Wells T, Frame V, Soffer B, Shaw W, Zhang
Z, Herrera P, et al. A double-blind, placebocontrolled, dose-response study of the effectiveness and safety of enalapril for children
with hypertension. J Clin Pharmacol
2002;42:870–80. F
119. Kavey RE, Daniels SR, Lauer RM, Atkins
DL, Hayman LL, Taubert K. American
Heart Association guidelines for primary prevention of atherosclerotic cardiovascular
disease beginning in childhood. Circulation
2003;107:1562–6. PR
128. Soffer B, Zhang Z, Miller K, Vogt BA,
Shahinfar S. A double-blind, placebocontrolled, dose-response study of the effectiveness and safety of lisinopril for children
with hypertension. Am J Hypertens
2003;16:795–800. RA
120. Blumenthal S, Epps RP, Heavenrich R, Lauer
RM, Lieberman E, Mirkin B, et al. Report of
the task force on blood pressure control in
children. Pediatrics 1977;59:797–820. PR
129. Sakarcan A, Tenney F, Wilson JT, Stewart JJ,
Adcock KG, Wells TG, et al. The pharmacokinetics of irbesartan in hypertensive children
and adolescents. J Clin Pharmacol
2001;41:742–9.
121. The Food and Drug Administration
Modernization Act of 1997. Public Law 105115. Enacted November 21, 1997.
122. Wells TG. Trials of antihypertensive therapies in children. Blood Press Monit
1999;4:189–92. PR
123. Flynn JT. Successes and shortcomings of the
Food and Drug Modernization Act. Am J
Hypertens 2003;16:889–91. PR
124. Best Pharmaceuticals for Children Act of
2002. Public Law 107-109. Enacted
January 4, 2002.
125. U.S. Department of Health and Human
Services, National Institutes of Health. List
of drugs for which pediatric studies are
needed. Federal Register 2003;68:2789–90.
130. Trachtman H, Frank R, Mahan JD, Portman
R, Restaino I, Matoo TK, et al. Clinical trial
of extended-release felodipine in pediatric
essential hypertension. Pediatr Nephrol
2003;18:548–53. RA
131. Sorof JM, Cargo P, Graepel J, Humphrey D,
King E, Rolf C, et al. Beta-blocker/thiazide
combination for treatment of hypertensive
children: A randomized double-blind,
placebo-controlled trial. Pediatr Nephrol
2002;17:345–50. RA
132. Adelman RD, Coppo R, Dillon MJ. The
emergency management of severe hypertension. Pediatr Nephrol 2000;14:422–7. PR
133. Vaughan CJ, Delanty N. Hypertensive emergencies. Lancet 2000;356:411–7. PR
References
47
134. Sheps SG, Roccella EJ. Reflections on the
sixth report of the Joint National Committee
on Prevention, Detection, Evaluation, and
Treatment of High Blood Pressure. Curr
Hypertens Rep 1999;1:342–5. PR
135. Ingelfinger JR. Renovascular disease in children. Kidney Int 1993;43:493–505. PR
136. World Health Organization. World Health
Report 2002: Reducing risks, promoting
healthy life. Geneva, Switzerland: 2002.
Available at: www.who.int/whr/2002/.
Verified July 12, 2004.
48
137. U.S. Department of Health and Human
Services, National Institutes of Health,
National Heart, Lung, and Blood Institute.
National High Blood Pressure Education
Program. Available at: www.nhlbi.nih.gov/
about/nhbpep/index.htm. Verified July 12,
2004.
138. JNC 6. National High Blood Pressure
Education Program. The Sixth Report of
the Joint National Committee on Prevention,
Detection, Evaluation, and Treatment of
High Blood Pressure. Arch Intern Med
1997;157:2413–46. PR
The Fourth Report on the Diagnosis, Evaluation, and Treatment of High Blood Pressure in Children and Adolescents
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